Pyran compound or at least one derivative thereof

ABSTRACT

The invention relates to pyran derivatives of the formula I  
                 
and to a process and intermediates for their preparation and derivatisation, and to the use thereof in liquid-crystalline media.

The invention relates to a pyran compound, or one or more derivatives thereof, to a process for their preparation and derivatisation, and to the use thereof in liquid-crystalline media.

Pyran derivatives play an important role in chemistry and pharmacy, inter alia as ingredients of natural and synthetic aroma substances, in medicaments and in liquid-crystalline materials. However, preparative access to many pyrans, in particular those with a 2,5-disubstitution, is currently limited and, is often restricted to derivatization of carbohydrates containing pyranose ring units. Many theoretically conceivable pyran derivatives are hitherto not accessible synthetically.

It is therefore an object of the present invention to provide novel pyran derivatives which have industrially useful properties or can serve as starting compounds for the efficient synthesis of further pyran derivatives.

This object is achieved by compounds of the general formula I

where

-   a, b, c, d and e are each, independently of one another, 0 or 1; -   W is —CH₂— or —C(═O)—; -   R¹¹ is H, an alkyl radical having from 1 to 15 carbon atoms which is     unsubstituted or mono- or polysubstituted, identically or     differently, by halogen or —CN, where, in addition, one or more CH₂     groups in this radical may be replaced by —C═C—, —CH═CH—, —O—, —S—,     —C(O)—O— and/or —O—C(O)— in such a way that hetero atoms (O and S)     are not linked directly to one another; -   R¹² is H, halogen, —CN, —NCS, aralkyl, O-aralkyl or an alkyl radical     having from 1 to 15 carbon atoms which is unsubstituted or mono- or     polysubstituted, identically or differently, by halogen or —CN,     where, in addition, one or more CH₂ groups in this radical may be     replaced by —C≡C—, —CH═CH—, —O—, —S—, —C(O)—O— and/or —O—C(O)— in     such a way that hetero atoms (O and S) are not linked directly to     one another; -   Z¹¹ is a single bond, —CH₂—, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂—, —CF₂CF₂—,     —CH═CH— or —C═C—; -   Z¹² is a single bond, —CH₂—, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂— or     —CF₂CF₂—; -   Z¹³, Z¹⁴ and Z¹⁵ are each, independently of one another, a single     bond, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂—, —CF₂CF₂—, —CH═CH—, —C≡C—,     —CH₂O—, —CF₂O—, —C(O)— or —C(O)—O—; -   A¹¹ and A¹², independently of one another, are or -   A¹³ and A¹⁴, independently of one another, are -   A¹⁵ is     or -   A¹⁵-R¹² together are -   Z¹³-[-A¹³-Z¹⁴-]_(c)-[-A¹⁴-Z¹⁵-]_(d)-[-A¹⁵-]_(e)-R¹² is     where R¹² is as defined above, and L¹⁷, L¹⁸ and L¹⁹, independently     of one another, are H or F; -   q is 0, 1, 2, 3 or 4; -   p is 0, 1, 2 or 3; -   R¹³ and R¹⁴, independently of one another, are an alkanyl radical     having from 1 to 7 carbon atoms or together are an alkylene bridge     having from 2 to 7 carbon atoms;     with the proviso     that, in the case of direct linking of Z¹³ and R¹² to give -Z³-R²,     R¹² is H, aralkyl, alkanyl or alkenyl if Z¹³ is —C(═O)—O— or     —C(═O)—, and Z¹³ is not —CH₂O— or —CF₂O—; -   that, in the case of direct linking of Z¹⁴ and R¹² to give -Z¹⁴-R¹²,     R¹² is H, aralkyl, alkanyl or alkenyl if Z¹⁴ is —C(═O)—O— or     —C(═O)—, and Z¹⁴ is not —CH₂O— or —CF₂O—; -   that, in the case of direct linking of Z¹⁵ and R¹² to give -Z¹⁵-R¹²,     R¹² is H, aralkyl, alkanyl or alkenyl if Z¹⁵ is —C(═O)—O— or     —C(═O)—, and Z¹⁵ is not —CH₂O— or —CF₂O—; -   that R¹¹ is not H if simultaneously a and b are both zero and Z¹² is     a single bond; -   that R¹¹ is not CH₃ if simultaneously a and b are both zero, Z¹² and     Z¹³ are each a single bond, W is —CH₂— and     -[-A¹³-Z¹⁴-]_(c)-[-A¹⁴-Z¹⁵-]_(d)-[-A¹⁵-]_(e)-R¹² is unsubstituted     phenyl.

On the basis of their properties, the compounds of the formula I according to the invention are used in liquid-crystalline media or serve as starting compounds for the efficient synthesis of further pyran compounds, in particular those having mesogenic properties. The compounds of the formula I according to the invention are preferably mesogenic, in particular liquid-crystalline.

In connection with the present invention, the term “alkyl”-unless defined otherwise elsewhere in this description or in the claims—denotes a straight-chain or branched aliphatic hydrocarbon radical having from 1 to 15 (i.e. 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14 or 15) carbon atoms; this radical is unsubstituted or mono- or polysubstituted by identical or different fluorine, chlorine, bromine, iodine and/or cyano radicals.

If this alkyl radical is a saturated radical, it is also referred to as “alkanyl”(C_(a)H_(2a+1)-, where a is an integer from 1 to 15 and one or more hydrogen atoms may be replaced by halogen, in particular fluorine, and/or cyano). Furthermore, the term “alkyl” also covers hydrocarbon radicals which are unsubstituted or correspondingly mono- or polysubstituted by identical or different F, Cl, Br, I and/or —CN radicals and in which, in addition, one or more CH₂ groups may be replaced by —O— (“alkoxy”, “oxaalkyl”), —S— (“thioalkyl”), —CH═CH— (“alkenyl”), —C≡C— (“alkynyl”), —CO—O— or —O—CO— in such a way that hetero atoms (O and S) are not linked directly to one another. Alkyl is preferably a straight-chain or branched, unsubstituted or substituted alkanyl, alkenyl or alkoxy radical having 1, 2, 3, 4, 5, 6, 7 or 8 carbon atoms. If alkyl is an alkanyl radical, this is preferably methyl, ethyl, n-propyl, i-propyl, n-butyl, i-butyl, t-butyl, n-pentyl, neopentyl, n-hexyl, n-heptyl, n-octyl; CF₃, CHF₂, CH₂F; CF₂CF₃. The alkanyl radical is particularly preferably straight-chain and unsubstituted or substituted by F.

Since, in accordance with the invention, one or more CH₂ groups in an alkyl radical may be replaced by —O—, the term “alkyl” also covers “alkoxy” or “oxaalkyl” radicals. Alkoxy is taken to mean an O-alkyl radical in which the oxygen atom is bonded directly to the group substituted by the alkoxy radical or to the substituted ring, and alkyl is as defined above; alkyl is preferably then alkanyl or alkenyl. Preferred alkoxy radicals are methoxy, ethoxy, propoxy, butoxy, pentoxy, hexoxy, heptoxy and octoxy, where each of these radicals may also be substituted by halogen or cyano, preferably by one or more fluorine atoms. Alkoxy is particularly preferably —OCH₃, —OC₂H₅, —O-n-C₃H₇, —O-n-C₄H₉, —O-t-C₄H₉, —OCF₃, —OCHF₂, —OCH₂F or —OCHFCHF₂.

In connection with the present invention, the term “oxaalkyl” denotes alkyl radicals in which at least one non-terminal CH₂ group has been replaced by —O— in such a way that no adjacent hetero atoms (O and S) are present. Oxaalkyl preferably covers straight-chain radicals of the formula —C_(a)H_(2a+1)—O—(CH₂)_(b)—, where a and b are each, independently of one another, 1, 2, 3, 4, 5, 6, 7, 8, 9 or 10; a is particularly preferably an integer from 1 to 6, and b is 1 or 2.

If one or more CH₂ groups in an alkyl radical as defined above have been replaced by sulfur, a “thioalkyl” radical is present. “Thioalkyl” preferably covers a straight-chain radical of the formula —C_(a)H_(2a+1)—S—(CH₂)_(b)—, where a is 1, 2, 3, 4, 5, 6, 7, 8, 9 or 10, and b is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9 or 10; a is particularly preferably an integer from 1 to 6, and b is 0, 1 or 2. The thioalkyl radical may likewise be substituted by F, Cl, Br, I and/or —CN and is preferably unsubstituted.

In connection with the present invention, the term “alkenyl” denotes an alkyl radical as defined above in which one or more —CH═CH— groups are present. If two —CH═CH— groups are present in the radical, this may also be referred to as “alkadienyl”. An alkenyl radical may contain from 2 to 15 (i.e. 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14 or 15) carbon atoms and is branched or preferably straight-chain. The radical is unsubstituted or mono- or polysubstituted by identical or different F, Cl, Br, I and/or CN radicals. Furthermore, one or more CH₂ groups may each, independently of one another, be replaced by —O—, —S—, —C≡C—, —CO—O— or —OC—O— in such a way that hetero atoms (O and S) are not bonded directly to one another. If the CH═CH group carries a radical other than hydrogen on the two carbon atoms, for example if it is a non-terminal group, the CH═CH group can exist in two configurations, namely as the E isomer and the Z isomer. In general, the E isomer (trans) is preferred. The alkenyl radical preferably contains 2, 3, 4, 5, 6 or 7 carbon atoms and is vinyl, 1 E-propenyl, 1 E-butenyl, 1 E-pentenyl, 1E-hexenyl, 1E-heptenyl, 2-propenyl, 2E-butenyl, 2E-pentenyl, 2E-hexenyl, 2E-heptenyl, 3-butenyl, 3E-pentenyl, 3E-hexenyl, 3E-heptenyl, 4-pentenyl, 4Z-hexenyl, 4E-hexenyl, 4Z-heptenyl, 5-hexenyl or 6-heptenyl. Particularly preferred alkenyl radicals are vinyl, 1 E-propenyl and 3E-butenyl.

If one or more CH₂ groups in an alkyl radical have been replaced by —C≡C—, an alkynyl radical is present. Replacement of one or more CH₂ groups by —CO—O— or —O—CO— is also possible. The following radicals are preferred here: acetoxy, propionyloxy, butyryloxy, pentanoyloxy, hexanoyloxy, acetoxymethyl, propionyloxymethyl, butyryloxymethyl, pentanoyloxymethyl, 2-acetoxyethyl, 2-propionyloxyethyl, 2-butyryloxyethyl, 2-acetoxypropyl, 3-propionyloxypropyl, 4-acetoxybutyl, methoxycarbonyl, ethoxycarbonyl, propoxycarbonyl, butoxycarbonyl, pentoxycarbonyl, methoxycarbonylmethyl, ethoxycarbonylmethyl, propoxycarbonylmethyl, butoxycarbonylmethyl, 2-(methoxycarbonyl)ethyl, 2-(ethoxycarbonyl)ethyl, 2-(propoxycarbonyl)ethyl, 3-(methoxycarbonyl)propyl, 3-(ethoxycarbonyl)propyl and 4-(methoxycarbonyl)butyl.

If a CH₂ group in an alkyl radical has been replaced by unsubstituted or substituted —CH═CH— and an adjacent CH₂ group has been replaced by —CO—O— or —O—CO—, this radical may be straight-chain or branched. It is preferably straight-chain and has from 4 to 13 carbon atoms. Accordingly, it is particularly preferably acryloyloxymethyl, 2-acryloyloxyethyl, 3-acryloyloxypropyl, 4-acryloyloxybutyl, 5-acryloyloxypentyl, 6-acryloyloxyhexyl, 7-acryloyloxyheptyl, 8-acryloyloxyoctyl, 9-acryloyloxynonyl, 10-acryloyloxydecyl, methacryloyloxymethyl, 2-methacryloyloxyethyl, 3-methacryloyloxypropyl, 4-methacryloyloxybutyl, 5-methacryloyloxypentyl, 6-methacryloyloxyhexyl, 7-methacryloyloxyheptyl, 8-methacryloyloxyoctyl or 9-methacryloyloxynonyl.

In connection with the present invention, the term “aralkyl” represents an arylalkyl radical, i.e. a radical in which an aryl substituent is linked to an atom, a chain, another radical or a functional group via an alkyl bridge. The term “O-aralkyl” represents an arylalkoxy radical, i.e. a radical in which an arylalkyl substituent is linked to an atom, a chain, another radical or a functional group via an oxygen atom. The term aryl substituent here is taken to mean an aromatic hydrocarbon having from 6 to 18 carbon atoms which is optionally substituted by halogen, nitro, alkanyl and/or alkoxy radicals, in particular a phenyl or naphthyl radical. The alkyl bridge is preferably a saturated hydrocarbon radical, in particular methylene (—CH₂—) or ethylene (—CH₂CH₂—). Preferred examples of an aralkyl radical are benzyl and phenethyl. Preferred examples of an O-aralkyl radical are O-benzyl (—O—CH₂-phenyl), O-phenethyl (—O—CH₂CH₂-phenyl) and O-(p-nitrobenzyl).

In accordance with the invention, “alkylene bridge” means an aliphatic hydrocarbon chain which is unbranched or branched and has the formula —C_(n)H_(2n)—, for example —CH₂CH₂—, —CH₂CH₂CH₂— or —CH₂C(CH₃)₂CH₂—.

In connection with the present invention, “halogen” covers fluorine, chlorine, bromine and iodine.

If radicals or substituents of the pyran derivatives according to the invention or the pyran derivatives according to the invention themselves can be in the form of optically active or stereoisomeric radicals, substituents or compounds since they have, for example, a center of asymmetry, these are also covered by the present invention. It goes without saying here that the pyran derivatives of the general formulae I and III according to the invention can be in isomerically pure form, for example as pure enantiomers, diastereomers, E or Z isomers, trans or cis isomers, or in the form of a mixture of a plurality of isomers in any desired ratio, for example in the form of a racemate, E/Z isomer mixture or cis/trans isomer mixture.

The compounds of the formula I according to the invention preferably contain a total of not more than four ring systems, including the central pyran ring, so that a+b+c+d+e is ≦3; particularly preferably 1≦a+b+c+d+e≦3, i.e. at least one further ring system and not more than three further ring systems are present besides the pyran ring. It is furthermore preferred for R¹¹ to be a straight-chain alkenyl or particularly preferably a straight-chain alkanyl radical having from 1 to 7 carbon atoms, in particular methyl, and for R¹² to be halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine.

Compounds of the formula I containing branched wing groups R¹¹ and/or R¹² may occasionally be of importance on use in liquid-crystalline media owing to their very good solubility in the usual liquid-crystalline base materials, but in particular as chiral dopants if they are optically active. Smectic compounds of this type are suitable as components of ferroelectric materials. Branched groups of this type generally contain not more than one chain branch. Preferred branched radicals R¹¹ and R¹² are isopropyl, 2-butyl (=1-methylpropyl), isobutyl (=2-methylpropyl), 2-methylbutyl, isopentyl (=3-methylbutyl), 2-methylpentyl, 3-methylpentyl, 2-ethylhexyl, 2-propylpentyl, isopropoxy, 2-methylpropoxy, 2-methylbutoxy, 3-methylbutoxy, 2-methylpentyloxy, 3-methylpentyloxy, 2-ethylhexyloxy, 1-methylhexyloxy and 1-methylheptyloxy.

A preferred class of compounds of the formula I according to the invention is formed by pyran derivatives in which W in the formula I is a carbonyl group, i.e. —C(═O)—. The compounds are then lactones of the general formula I-A:

where a, b, c, d, e, R¹¹, R¹², Z¹¹, Z¹², Z¹³, Z¹⁴, Z¹⁵, A¹¹, A¹², A¹³, A¹⁴ and A¹⁵ are as defined for the formula I above.

Another preferred class of compounds of the formula I according to the invention is formed by pyran derivatives in which W in the formula I is a methylene group, i.e. —CH₂—. The compounds are then dihydropyrans of the general formula I-B:

where a, b, c, d, e, R¹¹, R¹², Z¹¹, Z¹², Z¹³, Z¹⁴, Z¹⁵, A¹¹, A¹², A¹³, A¹⁴ and A¹⁵ are as defined for the formula I above.

In connection with the present invention, the compounds of the formula I according to the invention are also referred to as “pyran derivatives”; the term “pyran derivatives” covers both pyrans of the formula I-B and lactones of the formula I-A.

Preferred embodiments of the invention are furthermore compounds of the formula I in which Z¹² is a single bond and the central pyran ring is bonded either directly to R¹¹(a=b=0) or to ring A¹¹(a=1; b=0) or to ring A¹² (a=0; b=1) (formula. I-C):

where a, b, c, d, e, W, R¹¹, R¹², Z¹¹, Z¹³, Z¹⁴, Z¹⁵, A¹¹, A¹², A¹³, A¹⁴ and A¹⁵ are as defined for the formula I above. Preferred sub-groups of compounds of the formula I-C are formed here by compounds of the formula I-CA where W is —C(═O)— and in particular by compounds of the formula I-CB where W is —CH₂—:

where a, b, c, d, e, R¹¹, R¹² Z¹¹, Z¹³ Z ⁴ Z¹⁵, A¹¹, A¹² A¹³, A¹⁴ and A¹⁵ are as defined for the formula I above. Particular preference is given here to compounds in which a=b=0 and R¹¹ is alkanyl in the formula I-CA or I-CB.

Preferred compounds of the invention are in addition those in which b is 1, Z¹¹ is a single bond and A¹² is a 1,4-cyclohexylene ring (formula I-D):

where a, c, d, e, W, R¹¹, R¹², Z¹², Z¹³, Z¹⁴, Z¹⁵, A¹¹, A¹³, A¹⁴ and A¹⁵ are as defined for the formula I above.

Preferred sub-groups of compounds of the formula I-D are formed here by compounds of the formula I-DA where W is —C(═O)— and in particular by compounds of the formula I-DB where W is —CH₂—.

Particular preference is given here to compounds of the formula. I-DB in which furthermore Z¹² is a single bond (formula I-DBA):

where a, c, d, e, R¹¹, R¹², Z¹³, Z¹⁴, Z¹⁵, A¹¹, A¹³, A¹⁴ and A¹⁵ are as defined for the formula I above. It is very particularly preferred here for Z¹³ to be a single bond or —CF₂O—, c and d both simultaneously to be zero and A¹⁵ to be a 1,4-phenylene ring which is optionally mono- or polysubstituted by fluorine.

A further group of preferred compounds according to the invention is formed by compounds of the formula I-E, i.e. compounds of the formula I where a=1 and A¹¹=1,4-cyclohexylene:

where b, c, d, e, W, R¹¹, R¹², Z¹¹, Z¹², Z¹³, Z¹⁴, Z¹⁵, A¹², A¹³, A¹⁴ and A¹⁵ are as defined for the formula I above. Preferred sub-groups of compounds of the formula I-E are formed here by compounds of the formula I-EA where W is —C(═O)— and in particular by compounds of the formula W-EB where W is —CH₂—.

Particularly preferred compounds of the formula -EB here are compounds of the formulae I-EBA and I-EBB; very particular preference is given to compounds of the formula I-EBC:

where b, c, d, e, R¹¹, R¹², Z¹¹, Z¹², Z¹³, Z¹⁴, Z¹⁵, A¹², A¹³, A¹⁴ and A¹⁵ are as defined for the formula I above. It is preferred here for Z¹³ to be a single bond or —CF₂O—, c and d both simultaneously to be zero and A¹⁵ to be a 1,4-phenylene ring which is optionally mono- or polysubstituted by fluorine.

In addition, it is also preferred for Z¹³ in the formula I to be a single bond (formula I-F) or to be a carboxyl function (formula I-G) or a difluorooxymethylene bridge (formula I-H):

where a, b, c, d, e, W, R¹¹, R¹², Z¹¹, Z¹², Z¹⁴, Z¹⁵, A¹¹, A¹², A¹³, A¹⁴ and A¹⁵ are as defined for the formulae I, I-C, I-D and I-E above. Preferred subgroups of compounds of the formulae I-F, I-G and I-H are formed here by compounds of the formulae I-FA, I-GA and I-HA where W is —C(═O)— and in particular by compounds of the formulae I-FB, I-GB and I-HB where W is —CH₂—. It is particularly preferred here for Z¹² to be a single bond. If a and b are both simultaneously zero, R¹¹ is preferably an alkanyl radical having from 1 to seven carbon atoms. If a is 1, A¹¹ is preferably a 1,4-cyclo-hexylene ring. If b is 1, Z¹¹ is preferably a single bond and A¹² is likewise a 1,4-cyclohexylene ring.

The compounds of the formula I according to the invention furthermore preferably contain a ring A¹⁵, this ring particularly preferably being a 1,4-phenylene ring which is optionally substituted by fluorine in the 3- and/or 5-position (formula I-J):

where a, b, c, d, W, R¹¹, R¹², Z¹¹, Z¹², Z¹³, Z¹⁴, Z¹⁵, A¹¹, A¹², A¹³ and A¹⁴ are as defined for the formulae I, I-C, I-D, I-E, I-F, I-G and I-H above, and L¹¹ and L¹², independently of one another, are H or F. Preferred sub-groups of compounds of the formula I-J are formed here by compounds of the formula I-JA where W is —C(═O)— and in particular by compounds of the formula I-JB where W is —CH₂—. R¹² here is particularly preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine.

A further group of preferred compounds of the formula I according to the invention is formed by compounds in which A¹⁵-R¹² is

where R¹³ and R¹⁴ are as defined for the formula I above, and which are represented by the formulae I-K (cyclohexanones) and I-L (ketals):

where a, b, c, d, W, R¹¹, Z¹¹, Z¹², Z¹³, Z¹⁴, Z¹⁵, A¹¹, A¹², A¹³ and A¹⁴ are as defined for the formula I above, c and d in the formulae I-K and I-L are particularly preferably simultaneously zero.

A further group of preferred compounds of the formula I according to the invention is formed by compounds in which c is 1; Z¹⁴ is a single bond, —C(O)—O— or —CF₂O—; A¹³ is

and L¹³ and L¹⁴, independently of one another, are H or F. These compounds are represented by the formulae I-M, I-N, I-O, I-P, I-Q and I-R:

where a, b, d, e, R¹¹, R¹², Z¹¹, Z¹², Z¹³, A¹¹, A¹², A¹⁴ and A¹⁵ are as defined for the formula I above. Preferred sub-groups of compounds of the formulae I-M, I-N, I-O, I-P, I-Q and I-R are formed here by compounds of the formulae I-MA, I-NA, I-OA, I-PA, I-QA and I-RA where W is —C(═O)— and in particular by compounds of the formulae I-MB, I-NB, I-OB, I-PB, I-QB and I-RB where W is —CH₂—. It is particularly preferred here for Z¹³ to be a single bond, d to be zero and e to be 1, and A¹⁵ to be a 1,4-phenylene ring which is optionally mono- or polysubstituted by fluorine.

A further group of preferred compounds according to the invention is formed by compounds of the formulae I-S and I-T, i.e. compounds of the formula I in which d is 1; Z¹⁵ is —CF₂O—; A¹⁴ is

and L¹⁵ and L¹⁶, independently of one another, are H or F:

where a, b, c, R¹¹, R¹², Z¹¹, Z¹², Z¹³, Z¹⁴, A¹¹, A¹², A¹³ and A¹⁵ are as defined for the formula I above. It is particularly preferred for A¹⁵ in the formulae I-S and I-T to be

and for Z¹³ to be a single bond. It is furthermore preferred for the compounds of the formula I-S where c=1 for Z¹⁴ to be a single bond and for A¹³ to be

For the compounds of the formula I-T where c=1, it is preferred for Z¹⁴ to be a single bond and A¹³ to be

Preferred sub-groups of compounds of the formulae I-S and I-T are formed here by compounds of the formulae I-SA and I-TA where W is —C(═O)— and in particular by compounds of the formulae I-SB and I-TB where W is —CH₂—.

Very particularly preferred compounds of the formula I-CB according to the invention are those of the formulae I-CBI and I-CBII (which, inter alia, also represent embodiments of compounds of the formulae I-F, I-J, I-P, I-Q, I-R and I-T (1-CBI) and I-F, I-J, I-M, I-N and 1-0 (1-CBII) respectively):

in which L¹³ and L¹⁴, independently of one another, are H or F, and Rat, R¹², L¹¹, L¹² and Z¹⁴ are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or particularly preferably alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, in particular methyl, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine, and Z¹⁴ is preferably a single bond, a carboxyl group or a difluorooxymethylene bridge.

Illustrative compounds of the formulae I-CBI and I-CBII are shown by the formulae I-CBIa, I-CBIb, I-CBIc, I-CBIIa, I-CBIIb and I-CBIIc, where the preferred meaning of R¹² L¹¹, L¹², L¹³ and L¹⁴ as well as n is indicated in Tables 1 and 2 below:

A further group of very particularly preferred compounds of the formula I-CB are those of the formula I-CBIII:

where R¹¹ and Z¹⁴-R¹² are as defined for the formula I above, and L¹³ and L¹⁴, independently of one another, are H or F. Z¹⁴-R¹² here is preferably formed by substituents which simplify further functionalization or derivatization with formation of other compounds of the formula I according to the invention, for example through the introduction of further ring systems A¹⁴ and/or A¹⁵. Z¹⁴-R¹² is particularly preferably alkoxy or O-aralkyl, in particular O-t-butyl, O-benzyl or O-(p-nitrobenzyl); CO₂H; CO₂-alkanyl or CO₂-aralkyl, in particular CO₂-t-butyl or CO₂-benzyl; and (single bond)halogen, in particular —Br. R¹¹ is preferably a straight-chain alkenyl or alkanyl radical having up to 7 carbon atoms.

Illustrative compounds of the formula I-CBIII are those of the formulae I-CBIIa, I-CBIIIb and I-CBIIIc:

in which L¹³ and L¹⁴, independently of one another, are H or F, R^(12a) is t-butyl, benzyl or p-nitrobenzyl, R^(12b) is H, alkanyl having from 1 to 5 carbon atoms, or aralkyl, in particular H, t-butyl or benzyl, while C_(n)H_(2n+1) is a straight-chain alkanyl radical where n=1, 2, 3, 4, 5, 6 or 7.

Very particularly preferred compounds of the formula I-DBA according to the invention are those of the formulae I-DBAI, I-DBAII and I-DBAIII:

in which L¹³ and L¹⁴, independently of one another, are H or F, and R¹¹, R¹², L¹¹, L¹², Z¹³ and Z¹⁴ are as defined for the formula I above, where R¹¹ is preferably H, a straight-chain alkenyl (C_(n)H_(2n−1)) or particularly preferably alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, in particular methyl, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine, Z¹³ is preferably a single bond or CF₂O, and Z¹⁴ is preferably a single bond, a carboxyl group or a difluorooxymethylene bridge.

Illustrative compounds of the formulae I-DBAI, I-DBAII and I-DBAIII are shown by the formulae I-DBAla, I-DBAlb, I-DBAlIa, I-DBAIIb, I-DBAIIIa and I-DBAIIIb, where the preferred meaning of R¹², L¹¹, L¹², L¹³ and L¹⁴ as well as n (n is 0, 1, 2, 3, 4, 5, 6 or 7) is indicated in Tables 3 and 4 below:

Very particularly preferred compounds of the formula I-EBC according to the invention are those of the formula I-EBCI:

in which R¹¹ and R¹² are as defined for the formula I above, where R¹¹ is preferably H, a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine.

Illustrative compounds of the formula I-EBCI are shown by the formula I-EBCIa, where the preferred meaning of R¹², L¹¹ and L¹² as well as n (n is 0, 1, 2, 3, 4, 5, 6 or 7) is indicated in Table 3 below:

Very particularly preferred compounds of the formula I-GB according to the invention are, besides compounds of the formula I-GBI, also those of the formulae I-GBII and I-GBIII (which, inter alia, also represent embodiments of compounds of the formula I-J):

in which L¹³ and L¹⁴, independently of one another, are H or F, R^(12b) is as defined for R¹² for the formula I above, and R¹¹, R¹², L¹¹ and L¹² are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H₂₊₁) radical having from 1 to 7 carbon atoms, while R¹² for I-GBII and I-GBIII is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine; for I-GBI, R^(12b) is preferably H, alkanyl having from 1 to 5 carbon atoms or aralkyl, in particular H, tert-butyl or benzyl.

Illustrative compounds of the formula I-GBI are shown by the formula I-GBIa, where the preferred meaning of R^(12b) and n (n is 1, 2, 3, 4, 5, 6 or 7) is indicated below in Table 5. Illustrative compounds of the formulae I-GBII and I-GBIII are shown by the formulae I-GBIIa and I-GBIIIa, where the preferred meaning of R¹², L¹¹, L¹², L¹³ and L¹⁴ as well as n (n is 1, 2, 3, 4, 5, 6 or 7) is indicated in Tables 1 and 2 below:

Very particular preferred compounds of the formula I-HB according to the invention are those are of the formulae I-HBI and I-HBII (where the compounds of the formulae I-HBI and I-HBII are, inter alia, also embodiments of compounds of the formula I-J):

in which L¹³ and L¹⁴, independently of one another, are H or F, and R¹¹, R¹², L¹¹ and L¹² are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H₂₊₁) radical having from 1 to 7 carbon atoms, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine.

Illustrative compounds of the formulae I-HBI and I-HBII are shown by the formulae I-HBIa and I-HBIIa, where the preferred meaning of R¹², L¹¹, L¹², L¹³ and L¹⁴ as well as n (n is 1, 2, 3, 4, 5, 6 or 7) is indicated in Tables 1 and 2 below:

Very particularly preferred compounds of the formula I-KB according to the invention are those of the formulae I-KBI and I-KBII:

in which R¹¹ is as defined for the formula I above and is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, in the case of I-KBII also H. Illustrative compounds of the formulae I-KBI and I-KBII are those in which R¹¹ is a straight-chain alkanyl radical C_(n)H_(2n+1) where n=1, 2, 3, 4, 5, 6 or 7.

Very particularly preferred compounds of the formula I-LB according to the invention are those of the formulae I-LBI and I-LBII:

in which R¹¹ is as defined for the formula I above and is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, in the case of I-LBII also H. R¹³ and R¹⁴ are likewise as defined for the formula I above and are preferably both methyl or together —(CH₂)₃—. Illustrative compounds of the formulae I-LBI and I-LBII are those in which R¹¹ is a straight-chain alkanyl radical C_(n)H₂₊₁ where n=1, 2, 3, 4, 5, 6 or 7.

Very particularly preferred compounds of the formula I-MB according to the invention are those of the formulae I-MBA and I-MBB:

in which L¹³ and L¹⁴, independently of one another, are H or F, and R¹¹, R¹², L¹¹ and L¹² are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H₂₊₁) radical having from 1 to 7 carbon atoms, in the case of 1-MBB also H, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine.

Illustrative compounds of the formula I-MBA are compounds which are also represented by the formula I-CBIIa above, and illustrative compounds of the formula I-MBB are compounds which are also represented by the formula I-DBAIIIa above.

Very particularly preferred compounds of the formula I-NB according to the invention are those of the formulae I-NBA, I-NBB, I-NBC and I-NBD:

in which L¹³ and L¹⁴, independently of one another, are H or F, and R¹¹, R¹², L¹¹ and L¹² are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, in the case of 1-NBB and I-NBD also H, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine. R^(12b) has the same meaning as for the formula I-CBIIIb or I-GBIa above.

Illustrative compounds of the formula I-NBA are compounds which are also represented by the formula I-CBIIb above, and illustrative compounds of the formula I-NBC are compounds which are also represented by the formula I-CBIIb above. Illustrative compounds of the formula I-NBB are those which are shown by the formula I-NBBIa, where the meaning of R¹², L¹¹, L¹², L¹³ and L¹⁴ as well as n (n is 0, 1, 2, 3, 4, 5, 6 or 7) is indicated in Table 4 below:

Very particularly preferred compounds of the formula I-OB according to the invention are those of the formulae I-OBA and I-OBB:

in which L¹³ and L¹⁴, independently of one another, are H or F, and R¹¹, R¹², L¹¹ and L¹² are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H₂₊₁) radical having from 1 to 7 carbon atoms, in the case of I-OBB also H, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine.

Illustrative compounds of the formula I-OBA are compounds which are also represented by the formula I-CBIIc above, and illustrative compounds of the formula I-OBB are compounds which are also represented by the formula I-DBAIIIb above.

Very particularly preferred compounds of the formula I-PB according to the invention are those of the formulae I-PBA and I-PBB:

in which R¹¹, R¹², L¹¹ and L¹² are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, in the case of I-PBB also H, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine.

Illustrative compounds of the formula I-PBA are compounds which are also represented by the formula I-CBIa above, and illustrative compounds of the formula I-PBB are compounds which are also represented by the formula I-DBAIIa above.

Very particularly preferred compounds of the formula I-QB according to the invention are those of the formulae I-QBA, I-QBB and I-QBC:

in which R¹¹, R¹², L¹¹ and L¹² are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H²⁻¹) or in particular alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, in the case of I-QBB also H, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine. R^(12b) has the same meaning as for the formula I-CBIIIb above.

Illustrative compounds of the formula I-QBA are compounds which are also represented by the formula I-CBIb above. Illustrative compounds of the formula I-QBB are compounds which are shown by the formula I-QBBIa, where the meaning of R¹², L¹¹ and L¹² as well as n (n is 0, 1, 2, 3, 4, 5, 6 or 7) is indicated in Table 3 below:

Very particularly preferred compounds of the formula I-RB according to the invention are those of the formulae I-RBA and I-RBB:

in which R¹¹, R¹², L¹¹ and L¹² are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, in the case of I-RBB also H, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine.

Illustrative compounds of the formula I-RBA are compounds which are also represented by the formula I-CBIc above, and illustrative compounds of the formula I-RBB are compounds which are also represented by the formula I-DBAIIb above.

Very particularly preferred compounds of the formula I-SB according to the invention are those of the formulae I-SBA and I-SBB:

in which L¹³, L¹⁴, L¹⁵ and L¹⁶, independently of one another, are H or F, and R¹¹, R¹², L¹¹ and L¹² are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine.

Illustrative compounds of the formulae I-SBA and I-SBB are compounds which are shown by the formulae I-SBAIa and I-SBBIa respectively, where the meaning of R¹², L¹¹, L¹², L¹³, L¹⁴, L¹⁵ and L¹⁶ as well as n (n is 1, 2, 3, 4, 5, 6 or 7) is indicated in Tables 2 and 6 below:

Very particularly preferred compounds of the formula I-TB according to the invention are those of the formula I-TBA:

in which R¹¹, R¹², L¹¹ and L¹² are as defined for the formula I above, where R¹¹ is preferably a straight-chain alkenyl (C_(n)H_(2n−1)) or in particular alkanyl (C_(n)H_(2n+1)) radical having from 1 to 7 carbon atoms, while R¹² is preferably halogen, in particular fluorine, or an unbranched alkanyl or alkoxy radical having from 1 to 5 carbon atoms which is optionally mono- or polysubstituted by halogen, in particular fluorine.

Illustrative compounds of the formula I-TBA are compounds which are shown by the formula I-TBAIa, where the meaning of R¹², L¹¹ and L¹² as well as n (n is 1, 2, 3, 4, 5, 6 or 7) is indicated in Table 1 below: TABLE 1 I-TBAla

Compound I-CBla-/I-CBlb-/I-CBlc-/I-GBlla-/I-HBla-/I-TBAla No. n* R¹² L¹¹ L¹² -1 1 F H H -2 1 F F H -3 1 F F F -4 1 CF₃ H H -5 1 CF₃ F H -6 1 CF₃ F F -7 1 OCF₃ H H -8 1 OCF₃ F H -9 1 OCF₃ F F -10 1 OCHF₂ H H -11 1 OCHF₂ F H -12 1 OCHF₂ F F -13 1 -CN H H -14 1 -CN F H -15 1 -CN F F -16 2 F H H -17 2 F F H -18 2 F F F -19 2 CF₃ H H -20 2 CF₃ F H -21 2 CF₃ F F -22 2 OCF₃ H H -23 2 OCF₃ F H -24 2 OCF₃ F F -25 2 OCHF₂ H H -26 2 OCHF₂ F H -27 2 OCHF₂ F F -28 2 -CN H H -29 2 -CN F H -30 2 -CN F F -31 3 F H H -32 3 F F H -33 3 F F F -34 3 CF₃ H H -35 3 CF₃ F H -36 3 CF₃ F F -37 3 OCF₃ H H -38 3 OCF₃ F H -39 3 OCF₃ F F -40 3 OCHF₂ H H -41 3 OCHF₂ F H -42 3 OCHF₂ F F -43 3 -CN H H -44 3 -CN F H -45 3 -CN F F -46 4 F H H -47 4 F F H -48 4 F F F -49 4 CF₃ H H -50 4 CF₃ F H -51 4 CF₃ F F -52 4 OCF₃ H H -53 4 OCF₃ F H -54 4 OCF₃ F F -55 4 OCHF₂ H H -56 4 OCHF₂ F H -57 4 OCHF₂ F F -58 4 -CN H H -59 4 -CN F H -60 4 -CN F F -61 5 F H H -62 5 F F H -63 5 F F F -64 5 CF₃ H H -65 5 CF₃ F H -66 5 CF₃ F F -67 5 OCF₃ H H -68 5 OCF₃ F H -69 5 OCF₃ F F -70 5 OCHF₂ H H -71 5 OCHF₂ F H -72 5 OCHF₂ F F -73 5 -CN H H -74 5 -CN F H -75 5 -CN F F *: The radical C_(n)H_(2n+1) is unbranched.

TABLE 2 Compound I-CBIIa-/I-CBIIb-/ I-CBIIc-/I-GBIIIa-/ I-HBIIa-/I-SBAIa No. n* R¹² L¹¹ L¹² L¹³** L¹⁴*** −1 1 F H H H H −2 1 F F H H H −3 1 F F F H H −4 1 F F F F H −5 1 F F F F F −6 1 F F H F H −7 1 F F H F F −8 1 CF₃ H H H H −9 1 CF₃ F H H H −10 1 CF₃ F F H H −11 1 CF₃ F F F H −12 1 CF₃ F F F F −13 1 CF₃ F H F H −14 1 CF₃ F H F F −15 1 OCF₃ H H H H −16 1 OCF₃ F H H H −17 1 OCF₃ F F H H −18 1 OCF₃ F F F H −19 1 OCF₃ F F F F −20 1 OCF₃ F H F H −21 1 OCF₃ F H F F −22 1 OCHF₂ H H H H −23 1 OCHF₂ F H H H −24 1 OCHF₂ F F H H −25 1 OCHF₂ F F F H −26 1 OCHF₂ F F F F −27 1 OCHF₂ F H F H −28 1 OCHF₂ F H F F −29 1 —CN H H H H −30 1 —CN F H H H −31 1 —CN F F H H −32 1 —CN F F F H −33 1 —CN F F F F −34 1 —CN F H F H −35 1 —CN F H F F −36 2 F H H H H −37 2 F F H H H −38 2 F F F H H −39 2 F F F F H −40 2 F F F F F −41 2 F F H F H −42 2 F F H F F −43 2 CF₃ H H H H −44 2 CF₃ F H H H −45 2 CF₃ F F H H −46 2 CF₃ F F F H −47 2 CF₃ F F F F −48 2 CF₃ F H F H −49 2 CF₃ F H F F −50 2 OCF₃ H H H H −51 2 OCF₃ F H H H −52 2 OCF₃ F F H H −53 2 OCF₃ F F F H −54 2 OCF₃ F F F F −55 2 OCF₃ F H F H −56 2 OCF₃ F H F F −57 2 OCHF₂ H H H H −58 2 OCHF₂ F H H H −59 2 OCHF₂ F F H H −60 2 OCHF₂ F F F H −61 2 OCHF₂ F F F F −62 2 OCHF₂ F H F H −63 2 OCHF₂ F H F F −64 2 —CN H H H H −65 2 —CN F H H H −66 2 —CN F F H H −67 2 —CN F F F H −68 2 —CN F F F F −69 2 —CN F H F H −70 2 —CN F H F F −71 3 F H H H H −72 3 F F H H H −73 3 F F F H H −74 3 F F F F H −75 3 F F F F F −76 3 F F H F H −77 3 F F H F F −78 3 CF₃ H H H H −79 3 CF₃ F H H H −80 3 CF₃ F F H H −81 3 CF₃ F F F H −82 3 CF₃ F F F F −83 3 CF₃ F H F H −84 3 CF₃ F H F F −85 3 OCF₃ H H H H −86 3 OCF₃ F H H H −87 3 OCF₃ F F H H −88 3 OCF₃ F F F H −89 3 OCF₃ F F F F −90 3 OCF₃ F H F H −91 3 OCF₃ F H F F −92 3 OCHF₂ H H H H −93 3 OCHF₂ F H H H −94 3 OCHF₂ F F H H −95 3 OCHF₂ F F F H −96 3 OCHF₂ F F F F −97 3 OCHF₂ F H F H −98 3 OCHF₂ F H F F −99 3 —CN H H H H −100 3 —CN F H H H −101 3 —CN F F H H −102 3 —CN F F F H −103 3 —CN F F F F −104 3 —CN F H F H −105 3 —CN F H F F −106 4 F H H H H −107 4 F F H H H −108 4 F F F H H −109 4 F F F F H −110 4 F F F F F −111 4 F F H F H −112 4 F F H F F −113 4 CF₃ H H H H −114 4 CF₃ F H H H −115 4 CF₃ F F H H −116 4 CF₃ F F F H −117 4 CF₃ F F F F −118 4 CF₃ F H F H −119 4 CF₃ F H F F −120 4 OCF₃ H H H H −121 4 OCF₃ F H H H −122 4 OCF₃ F F H H −123 4 OCF₃ F F F H −124 4 OCF₃ F F F F −125 4 OCF₃ F H F H −126 4 OCF₃ F H F F −127 4 OCHF₂ H H H H −128 4 OCHF₂ F H H H −129 4 OCHF₂ F F H H −130 4 OCHF₂ F F F H −131 4 OCHF₂ F F F F −132 4 OCHF₂ F H F H −133 4 OCHF₂ F H F F −134 4 —CN H H H H −135 4 —CN F H H H −136 4 —CN F F H H −137 4 —CN F F F H −138 4 —CN F F F F −139 4 —CN F H F H −140 4 —CN F H F F −141 5 F H H H H −142 5 F F H H H −143 5 F F F H H −144 5 F F F F H −145 5 F F F F F −146 5 F F H F H −147 5 F F H F F −148 5 CF₃ H H H H −149 5 CF₃ F H H H −150 5 CF₃ F F H H −151 5 CF₃ F F F H −152 5 CF₃ F F F F −153 5 CF₃ F H F H −154 5 CF₃ F H F F −155 5 OCF₃ H H H H −156 5 OCF₃ F H H H −157 5 OCF₃ F F H H −158 5 OCF₃ F F F H −159 5 OCF₃ F F F F −160 5 OCF₃ F H F H −161 5 OCF₃ F H F F −162 5 OCHF₂ H H H H −163 5 OCHF₂ F H H H −164 5 OCHF₂ F F H H −165 5 OCHF₂ F F F H −166 5 OCHF₂ F F F F −167 5 OCHF₂ F H F H −168 5 OCHF₂ F H F F −169 5 —CN H H H H −170 5 —CN F H H H −171 5 —CN F F H H −172 5 —CN F F F H −173 5 —CN F F F F −174 5 —CN F H F H −175 5 —CN F H F F *The radical C_(n)H_(2n+1) is unbranched. **L¹⁵ for the compounds of the formula I-SBAIa ***L¹⁶ for the compounds of the formula I-SBAIa

TABLE 3 Compound I-DBAIa-/I-DBAIb-/I-DBAIIa- /I-DBAIIb-/I-EBCIa- /I-QBBIa No. n* R¹² L¹¹ L¹² −1 0 F H H −2 0 F F H −3 0 F F F −4 0 CF₃ H H −5 0 CF₃ F H −6 0 CF₃ F F −7 0 OCF₃ H H −8 0 OCF₃ F H −9 0 OCF₃ F F −10 0 OCHF₂ H H −11 0 OCHF₂ F H −12 0 OCHF₂ F F −13 0 —CN H H −14 0 —CN F H −15 0 —CN F F −16 1 F H H −17 1 F F H −18 1 F F F −19 1 CF₃ H H −20 1 CF₃ F H −21 1 CF₃ F F −22 1 OCF₃ H H −23 1 OCF₃ F H −24 1 OCF₃ F F −25 1 OCHF₂ H H −26 1 OCHF₂ F H −27 1 OCHF₂ F F −28 1 —CN H H −29 1 —CN F H −30 1 —CN F F −31 2 F H H −32 2 F F H −33 2 F F F −34 2 CF₃ H H −35 2 CF₃ F H −36 2 CF₃ F F −37 2 OCF₃ H H −38 2 OCF₃ F H −39 2 OCF₃ F F −40 2 OCHF₂ H H −41 2 OCHF₂ F H −42 2 OCHF₂ F F −43 2 —CN H H −44 2 —CN F H −45 2 —CN F F −46 3 F H H −47 3 F F H −48 3 F F F −49 3 CF₃ H H −50 3 CF₃ F H −51 3 CF₃ F F −52 3 OCF₃ H H −53 3 OCF₃ F H −54 3 OCF₃ F F −55 3 OCHF₂ H H −56 3 OCHF₂ F H −57 3 OCHF₂ F F −58 3 —CN H H −59 3 —CN F H −60 3 —CN F F −61 4 F H H −62 4 F F H −63 4 F F F −64 4 CF₃ H H −65 4 CF₃ F H −66 4 CF₃ F F −67 4 OCF₃ H H −68 4 OCF₃ F H −69 4 OCF₃ F F −70 4 OCHF₂ H H −71 4 OCHF₂ F H −72 4 OCHF₂ F F −73 4 —CN H H −74 4 —CN F H −75 4 —CN F F −76 5 F H H −77 5 F F H −78 5 F F F −79 5 CF₃ H H −80 5 CF₃ F H −81 5 CF₃ F F −82 5 OCF₃ H H −83 5 OCF₃ F H −84 5 OCF₃ F F −85 5 OCHF₂ H H −86 5 OCHF₂ F H −87 5 OCHF₂ F F −88 5 —CN H H −89 5 —CN F H −90 5 —CN F F *The radical C_(n)H_(2n+1) is unbranched.

TABLE 4 Compound I-DBAIIIa-/I-DBAIIIb-/ I-NBBIa No. n* R¹² L¹¹ L¹² L¹³ L¹⁴ −1 0 F H H H H −2 0 F F H H H −3 0 F F F H H −4 0 F F F F H −5 0 F F F F F −6 0 F F H F H −7 0 F F H F F −8 0 CF₃ H H H H −9 0 CF₃ F H H H −10 0 CF₃ F F H H −11 0 CF₃ F F F H −12 0 CF₃ F F F F −13 0 CF₃ F H F H −14 0 CF₃ F H F F −15 0 OCF₃ H H H H −16 0 OCF₃ F H H H −17 0 OCF₃ F F H H −18 0 OCF₃ F F F H −19 0 OCF₃ F F F F −20 0 OCF₃ F H F H −21 0 OCF₃ F H F F −22 0 OCHF₂ H H H H −23 0 OCHF₂ F H H H −24 0 OCHF₂ F F H H −25 0 OCHF₂ F F F H −26 0 OCHF₂ F F F F −27 0 OCHF₂ F H F H −28 0 OCHF₂ F H F F −29 0 —CN H H H H −30 0 —CN F H H H −31 0 —CN F F H H −32 0 —CN F F F H −33 0 —CN F F F F −34 0 —CN F H F H −35 0 —CN F H F F −36 1 F H H H H −37 1 F F H H H −38 1 F F F H H −39 1 F F F F H −40 1 F F F F F −41 1 F F H F H −42 1 F F H F F −43 1 CF₃ H H H H −44 1 CF₃ F H H H −45 1 CF₃ F F H H −46 1 CF₃ F F F H −47 1 CF₃ F F F F −48 1 CF₃ F H F H −49 1 CF₃ F H F F −50 1 OCF₃ H H H H −51 1 OCF₃ F H H H −52 1 OCF₃ F F H H −53 1 OCF₃ F F F H −54 1 OCF₃ F F F F −55 1 OCF₃ F H F H −56 1 OCF₃ F H F F −57 1 OCHF₂ H H H H −58 1 OCHF₂ F H H H −59 1 OCHF₂ F F H H −60 1 OCHF₂ F F F H −61 1 OCHF₂ F F F F −62 1 OCHF₂ F H F H −63 1 OCHF₂ F H F F −64 1 —CN H H H H −65 1 —CN F H H H −66 1 —CN F F H H −67 1 —CN F F F H −68 1 —CN F F F F −69 1 —CN F H F H −70 1 —CN F H F F −71 2 F H H H H −72 2 F F H H H −73 2 F F F H H −74 2 F F F F H −75 2 F F F F F −76 2 F F H F H −77 2 F F H F F −78 2 CF₃ H H H H −79 2 CF₃ F H H H −80 2 CF₃ F F H H −81 2 CF₃ F F F H −82 2 CF₃ F F F F −83 2 CF₃ F H F H −84 2 CF₃ F H F F −85 2 OCF₃ H H H H −86 2 OCF₃ F H H H −87 2 OCF₃ F F H H −88 2 OCF₃ F F F H −89 2 OCF₃ F F F F −90 2 OCF₃ F H F H −91 2 OCF₃ F H F F −92 2 OCHF₂ H H H H −93 2 OCHF₂ F H H H −94 2 OCHF₂ F F H H −95 2 OCHF₂ F F F H −96 2 OCHF₂ F F F F −97 2 OCHF₂ F H F H −98 2 OCHF₂ F H F F −99 2 —CN H H H H −100 2 —CN F H H H −101 2 —CN F F H H −102 2 —CN F F F H −103 2 —CN F F F F −104 2 —CN F H F H −105 2 —CN F H F F −106 3 F H H H H −107 3 F F H H H −108 3 F F F H H −109 3 F F F F H −110 3 F F F F F −111 3 F F H F H −112 3 F F H F F −113 3 CF₃ H H H H −114 3 CF₃ F H H H −115 3 CF₃ F F H H −116 3 CF₃ F F F H −117 3 CF₃ F F F F −118 3 CF₃ F H F H −119 3 CF₃ F H F F −120 3 OCF₃ H H H H −121 3 OCF₃ F H H H −122 3 OCF₃ F F H H −123 3 OCF₃ F F F H −124 3 OCF₃ F F F F −125 3 OCF₃ F H F H −126 3 OCF₃ F H F F −127 3 OCHF₂ H H H H −128 3 OCHF₂ F H H H −129 3 OCHF₂ F F H H −130 3 OCHF₂ F F F H −131 3 OCHF₂ F F F F −132 3 OCHF₂ F H F H −133 3 OCHF₂ F H F F −134 3 —CN H H H H −135 3 —CN F H H H −136 3 —CN F F H H −137 3 —CN F F F H −138 3 —CN F F F F −139 3 —CN F H F H −140 3 —CN F H F F −141 4 F H H H H −142 4 F F H H H −143 4 F F F H H −144 4 F F F F H −145 4 F F F F F −146 4 F F H F H −147 4 F F H F F −148 4 CF₃ H H H H −149 4 CF₃ F H H H −150 4 CF₃ F F H H −151 4 CF₃ F F F H −152 4 CF₃ F F F F −153 4 CF₃ F H F H −154 4 CF₃ F H F F −155 4 OCF₃ H H H H −156 4 OCF₃ F H H H −157 4 OCF₃ F F H H −158 4 OCF₃ F F F H −159 4 OCF₃ F F F F −160 4 OCF₃ F H F H −161 4 OCF₃ F H F F −162 4 OCHF₂ H H H H −163 4 OCHF₂ F H H H −164 4 OCHF₂ F F H H −165 4 OCHF₂ F F F H −166 4 OCHF₂ F F F F −167 4 OCHF₂ F H F H −168 4 OCHF₂ F H F F −169 4 —CN H H H H −170 4 —CN F H H H −171 4 —CN F F H H −172 4 —CN F F F H −173 4 —CN F F F F −174 4 —CN F H F H −175 4 —CN F H F F −176 5 F H H H H −177 5 F F H H H −178 5 F F F H H −179 5 F F F F H −180 5 F F F F F −181 5 F F H F H −182 5 F F H F F −183 5 CF₃ H H H H −184 5 CF₃ F H H H −185 5 CF₃ F F H H −186 5 CF₃ F F F H −187 5 CF₃ F F F F −188 5 CF₃ F H F H −189 5 CF₃ F H F F −190 5 OCF₃ H H H H −191 5 OCF₃ F H H H −192 5 OCF₃ F F H H −193 5 OCF₃ F F F H −194 5 OCF₃ F F F F −195 5 OCF₃ F H F H −196 5 OCF₃ F H F F −197 5 OCHF₂ H H H H −198 5 OCHF₂ F H H H −199 5 OCHF₂ F F H H −200 5 OCHF₂ F F F H −201 5 OCHF₂ F F F F −202 5 OCHF₂ F H F H −203 5 OCHF₂ F H F F −204 5 —CN H H H H −205 5 —CN F H H H −206 5 —CN F F H H −207 5 —CN F F F H −208 5 —CN F F F F −209 5 —CN F H F H −210 5 —CN F H F F

TABLE 5 Compound Compound I-GBIa n* R^(12b) I-GBIa n* R^(12b) −1 0 H −2 0 CH₃ −3 0 C₂H₅ −4 0 n-C₃H₇ −5 0 t-C₄H₉ −6 0 CH₂-phenyl −7 1 H −8 1 CH₃ −9 1 C₂H₅ −10 1 n-C₃H₇ −11 1 t-C₄H₉ −12 1 CH₂-phenyl −13 3 H −14 3 CH₃ −15 3 C₂H₅ −16 3 n-C₃H₇ −17 3 t-C₄H₉ −18 3 CH₂-phenyl −19 5 H −20 5 CH₃ −21 5 C₂H₅ −22 5 n-C₃H₇ −23 5 t-C₄H₉ −24 5 CH₂-phenyl *The radical C_(n)H_(2n+1) is unbranched.

TABLE 6 Compound I-SBBIa No. n* R¹² L¹¹ L¹² L¹⁵ L¹⁶ L¹³ L¹⁴ −1 1 F H H H H H H −2 1 F F H H H H H −3 1 F F F H H H H −4 1 F F F F H H H −5 1 F F F F F H H −6 1 F F H F H H H −7 1 F F H F F H H −8 1 F H H H H F H −9 1 F F H H H F H −10 1 F F F H H F H −11 1 F F F F H F H −12 1 F F F F F F H −13 1 F F H F H F H −14 1 F F H F F F H −15 1 CF₃ H H H H H H −16 1 CF₃ F H H H H H −17 1 CF₃ F F H H H H −18 1 CF₃ F F F H H H −19 1 CF₃ F F F F H H −20 1 CF₃ F H F H H H −21 1 CF₃ F H F F H H −22 1 CF₃ H H H H F H −23 1 CF₃ F H H H F H −24 1 CF₃ F F H H F H −25 1 CF₃ F F F H F H −26 1 CF₃ F F F F F H −27 1 CF₃ F H F H F H −28 1 CF₃ F H F F F H −29 1 OCF₃ H H H H H H −30 1 OCF₃ F H H H H H −31 1 OCF₃ F F H H H H −32 1 OCF₃ F F F H H H −33 1 OCF₃ F F F F H H −34 1 OCF₃ F H F H H H −35 1 OCF₃ F H F F H H −36 1 OCF₃ H H H H F H −37 1 OCF₃ F H H H F H −38 1 OCF₃ F F H H F H −39 1 OCF₃ F F F H F H −40 1 OCF₃ F F F F F H −41 1 OCF₃ F H F H F H −42 1 OCF₃ F H F F F H −43 1 OCHF₂ H H H H H H −44 1 OCHF₂ F H H H H H −45 1 OCHF₂ F F H H H H −46 1 OCHF₂ F F F H H H −47 1 OCHF₂ F F F F H H −48 1 OCHF₂ F H F H H H −49 1 OCHF₂ F H F F H H −50 1 OCHF₂ H H H H F H −51 1 OCHF₂ F H H H F H −52 1 OCHF₂ F F H H F H −53 1 OCHF₂ F F F H F H −54 1 OCHF₂ F F F F F H −55 1 OCHF₂ F H F H F H −56 1 OCHF₂ F H F F F H −57 1 —CN H H H H H H −58 1 —CN F H H H H H −59 1 —CN F F H H H H −60 1 —CN F F F H H H −61 1 —CN F F F F H H −62 1 —CN F H F H H H −63 1 —CN F H F F H H −64 1 —CN H H H H F H −65 1 —CN F H H H F H −66 1 —CN F F H H F H −67 1 —CN F F F H F H −68 1 —CN F F F F F H −69 1 —CN F H F H F H −70 1 —CN F H F F F H −71 2 F H H H H H H −72 2 F F H H H H H −73 2 F F F H H H H −74 2 F F F F H H H −75 2 F F F F F H H −76 2 F F H F H H H −77 2 F F H F F H H −78 2 F H H H H F H −79 2 F F H H H F H −80 2 F F F H H F H −81 2 F F F F H F H −82 2 F F F F F F H −83 2 F F H F H F H −84 2 F F H F F F H −85 2 CF₃ H H H H H H −86 2 CF₃ F H H H H H −87 2 CF₃ F F H H H H −88 2 CF₃ F F F H H H −89 2 CF₃ F F F F H H −90 2 CF₃ F H F H H H −91 2 CF₃ F H F F H H −92 2 CF₃ H H H H F H −93 2 CF₃ F H H H F H −94 2 CF₃ F F H H F H −95 2 CF₃ F F F H F H −96 2 CF₃ F F F F F H −97 2 CF₃ F H F H F H −98 2 CF₃ F H F F F H −99 2 OCF₃ H H H H H H −100 2 OCF₃ F H H H H H −101 2 OCF₃ F F H H H H −102 2 OCF₃ F F F H H H −103 2 OCF₃ F F F F H H −104 2 OCF₃ F H F H H H −105 2 OCF₃ F H F F H H −106 2 OCF₃ H H H H F H −107 2 OCF₃ F H H H F H −108 2 OCF₃ F F H H F H −109 2 OCF₃ F F F H F H −110 2 OCF₃ F F F F F H −111 2 OCF₃ F H F H F H −112 2 OCF₃ F H F F F H −113 2 OCHF₂ H H H H H H −114 2 OCHF₂ F H H H H H −115 2 OCHF₂ F F H H H H −116 2 OCHF₂ F F F H H H −117 2 OCHF₂ F F F F H H −118 2 OCHF₂ F H F H H H −119 2 OCHF₂ F H F F H H −120 2 OCHF₂ H H H H F H −121 2 OCHF₂ F H H H F H −122 2 OCHF₂ F F H H F H −123 2 OCHF₂ F F F H F H −124 2 OCHF₂ F F F F F H −125 2 OCHF₂ F H F H F H −126 2 OCHF₂ F H F F F H −127 2 —CN H H H H H H −128 2 —CN F H H H H H −129 2 —CN F F H H H H −130 2 —CN F F F H H H −131 2 —CN F F F F H H −132 2 —CN F H F H H H −133 2 —CN F H F F H H −134 2 —CN H H H H F H −135 2 —CN F H H H F H −136 2 —CN F F H H F H −137 2 —CN F F F H F H −138 2 —CN F F F F F H −139 2 —CN F H F H F H −140 2 —CN F H F F F H −141 3 F H H H H H H −142 3 F F H H H H H −143 3 F F F H H H H −144 3 F F F F H H H −145 3 F F F F F H H −146 3 F F H F H H H −147 3 F F H F F H H −148 3 F H H H H F H −149 3 F F H H H F H −150 3 F F F H H F H −151 3 F F F F H F H −152 3 F F F F F F H −153 3 F F H F H F H −154 3 F F H F F F H −155 3 CF₃ H H H H H H −156 3 CF₃ F H H H H H −157 3 CF₃ F F H H H H −158 3 CF₃ F F F H H H −159 3 CF₃ F F F F H H −160 3 CF₃ F H F H H H −161 3 CF₃ F H F F H H −162 3 CF₃ H H H H F H −163 3 CF₃ F H H H F H −164 3 CF₃ F F H H F H −165 3 CF₃ F F F H F H −166 3 CF₃ F F F F F H −167 3 CF₃ F H F H F H −168 3 CF₃ F H F F F H −169 3 OCF₃ H H H H H H −170 3 OCF₃ F H H H H H −171 3 OCF₃ F F H H H H −172 3 OCF₃ F F F H H H −173 3 OCF₃ F F F F H H −174 3 OCF₃ F H F H H H −175 3 OCF₃ F H F F H H −176 3 OCF₃ H H H H F H −177 3 OCF₃ F H H H F H −178 3 OCF₃ F F H H F H −179 3 OCF₃ F F F H F H −180 3 OCF₃ F F F F F H −181 3 OCF₃ F H F H F H −182 3 OCF₃ F H F F F H −183 3 OCHF₂ H H H H H H −184 3 OCHF₂ F H H H H H −185 3 OCHF₂ F F H H H H −186 3 OCHF₂ F F F H H H −187 3 OCHF₂ F F F F H H −188 3 OCHF₂ F H F H H H −189 3 OCHF₂ F H F F H H −190 3 OCHF₂ H H H H F H −191 3 OCHF₂ F H H H F H −192 3 OCHF₂ F F H H F H −193 3 OCHF₂ F F F H F H −194 3 OCHF₂ F F F F F H −195 3 OCHF₂ F H F H F H −196 3 OCHF₂ F H F F F H −197 3 —CN H H H H H H −198 3 —CN F H H H H H −199 3 —CN F F H H H H −200 3 —CN F F F H H H −201 3 —CN F F F F H H −202 3 —CN F H F H H H −203 3 —CN F H F F H H −204 3 —CN H H H H F H −205 3 —CN F H H H F H −206 3 —CN F F H H F H −207 3 —CN F F F H F H −208 3 —CN F F F F F H −209 3 —CN F H F H F H −210 3 —CN F H F F F H −211 4 F H H H H H H −212 4 F F H H H H H −213 4 F F F H H H H −214 4 F F F F H H H −215 4 F F F F F H H −216 4 F F H F H H H −217 4 F F H F F H H −218 4 F H H H H F H −219 4 F F H H H F H −220 4 F F F H H F H −221 4 F F F F H F H −222 4 F F F F F F H −223 4 F F H F H F H −224 4 F F H F F F H −225 4 CF₃ H H H H H H −226 4 CF₃ F H H H H H −227 4 CF₃ F F H H H H −228 4 CF₃ F F F H H H −229 4 CF₃ F F F F H H −230 4 CF₃ F H F H H H −231 4 CF₃ F H F F H H −232 4 CF₃ H H H H F H −233 4 CF₃ F H H H F H −234 4 CF₃ F F H H F H −235 4 CF₃ F F F H F H −236 4 CF₃ F F F F F H −237 4 CF₃ F H F H F H −238 4 CF₃ F H F F F H −239 4 OCF₃ H H H H H H −240 4 OCF₃ F H H H H H −241 4 OCF₃ F F H H H H −242 4 OCF₃ F F F H H H −243 4 OCF₃ F F F F H H −244 4 OCF₃ F H F H H H −245 4 OCF₃ F H F F H H −246 4 OCF₃ H H H H F H −247 4 OCF₃ F H H H F H −248 4 OCF₃ F F H H F H −249 4 OCF₃ F F F H F H −250 4 OCF₃ F F F F F H −251 4 OCF₃ F H F H F H −252 4 OCF₃ F H F F F H −253 4 OCHF₂ H H H H H H −254 4 OCHF₂ F H H H H H −255 4 OCHF₂ F F H H H H −256 4 OCHF₂ F F F H H H −257 4 OCHF₂ F F F F H H −258 4 OCHF₂ F H F H H H −259 4 OCHF₂ F H F F H H −260 4 OCHF₂ H H H H F H −261 4 OCHF₂ F H H H F H −262 4 OCHF₂ F F H H F H −263 4 OCHF₂ F F F H F H −264 4 OCHF₂ F F F F F H −265 4 OCHF₂ F H F H F H −266 4 OCHF₂ F H F F F H −267 4 —CN H H H H H H −268 4 —CN F H H H H H −269 4 —CN F F H H H H −270 4 —CN F F F H H H −271 4 —CN F F F F H H −272 4 —CN F H F H H H −273 4 —CN F H F F H H −274 4 —CN H H H H F H −275 4 —CN F H H H F H −276 4 —CN F F H H F H −277 4 —CN F F F H F H −278 4 —CN F F F F F H −279 4 —CN F H F H F H −280 4 —CN F H F F F H −281 5 F H H H H H H −282 5 F F H H H H H −283 5 F F F H H H H −284 5 F F F F H H H −285 5 F F F F F H H −286 5 F F H F H H H −287 5 F F H F F H H −288 5 F H H H H F H −289 5 F F H H H F H −290 5 F F F H H F H −291 5 F F F F H F H −292 5 F F F F F F H −293 5 F F H F H F H −294 5 F F H F F F H −295 5 CF₃ H H H H H H −296 5 CF₃ F H H H H H −297 5 CF₃ F F H H H H −298 5 CF₃ F F F H H H −299 5 CF₃ F F F F H H −300 5 CF₃ F H F H H H −301 5 CF₃ F H F F H H −302 5 CF₃ H H H H F H −303 5 CF₃ F H H H F H −304 5 CF₃ F F H H F H −305 5 CF₃ F F F H F H −306 5 CF₃ F F F F F H −307 5 CF₃ F H F H F H −308 5 CF₃ F H F F F H −309 5 OCF₃ H H H H H H −310 5 OCF₃ F H H H H H −311 5 OCF₃ F F H H H H −312 5 OCF₃ F F F H H H −313 5 OCF₃ F F F F H H −314 5 OCF₃ F H F H H H −315 5 OCF₃ F H F F H H −316 5 OCF₃ H H H H F H −317 5 OCF₃ F H H H F H −318 5 OCF₃ F F H H F H −319 5 OCF₃ F F F H F H −320 5 OCF₃ F F F F F H −321 5 OCF₃ F H F H F H −322 5 OCF₃ F H F F F H −323 5 OCHF₂ H H H H H H −324 5 OCHF₂ F H H H H H −325 5 OCHF₂ F F H H H H −326 5 OCHF₂ F F F H H H −327 5 OCHF₂ F F F F H H −328 5 OCHF₂ F H F H H H −329 5 OCHF₂ F H F F H H −330 5 OCHF₂ H H H H F H −331 5 OCHF₂ F H H H F H −332 5 OCHF₂ F F H H F H −333 5 OCHF₂ F F F H F H −334 5 OCHF₂ F F F F F H −335 5 OCHF₂ F H F H F H −336 5 OCHF₂ F H F F F H −337 5 —CN H H H H H H −338 5 —CN F H H H H H −339 5 —CN F F H H H H −340 5 —CN F F F H H H −341 5 —CN F F F F H H −342 5 —CN F H F H H H −343 5 —CN F H F F H H −344 5 —CN H H H H F H −345 5 —CN F H H H F H −346 5 —CN F F H H F H −347 5 —CN F F F H F H −348 5 —CN F F F F F H −349 5 —CN F H F H F H −350 5 —CN F H F F F H *The radical C_(n)H_(2n+1) is unbranched.

A further subject-matter according to the invention is a process for the preparation of pyran derivatives, in particular of the general formula I.

The process according to the invention is characterized in that it includes, as one process step, a ring-closing metathesis reaction of a compound of the general formula II

to give a pyran derivative of the formula I

in the presence of a metathesis catalyst, where a, b, c, d, e, W, R¹¹, R¹², Z¹¹, Z¹², Z¹³, Z¹⁴, Z¹⁵, A¹¹, A¹², A¹³, A¹⁴ and A¹⁵ in the formulae I and II are as defined for the formula I above; with the proviso that, in the case of direct linking of Z¹³ and R¹² to give -Z¹³-R¹² R¹² is H, aralkyl or alkanyl if Z¹³ is —C(═O)—, R¹² is aralkyl or alkanyl if Z¹³ is —C(═O)—O—, and Z¹³ is not —CH₂O— or —CF₂O—; that, in the case of direct linking of Z¹⁴ and R¹² to give -Z⁴-R¹², R¹² is H, aralkyl or alkanyl if Z¹⁴ is —C(═O)—, R¹² is aralkyl or alkanyl if Z¹⁴ is —C(═O)—O—, and Z¹⁴ is not —CH₂O— or —CF₂O—; that, in the case of direct linking of Z¹⁵ and R¹² to give -Z¹⁵-R¹², R¹² is H, aralkyl or alkanyl if Z¹⁵ is —C(═O)—, R¹² is aralkyl or alkanyl if Z¹⁵ is —C(═O)—O—, and Z¹⁵ is not —CH₂O— or —CF₂O—; that R¹¹ is not H if a and b are both simultaneously zero and Z¹² is a single bond; that R¹¹ is not CH₃ if simultaneously a and b are both zero, Z¹² and Z¹³ are each a single bond, W is —CH₂— and -[-A¹³-Z¹⁴-]_(c)-[-A¹⁴-Z¹⁵]_(d)-[-A¹⁵-]_(e)-R¹² is unsubstituted phenyl.

Metathesis reactions (frequently also known as olefin metathesis) for the synthesis of carbocyclic compounds (or of (poly)olefins from carbocyclic compounds) are well known in the prior art (see, inter alia, R. H. Grubbs and S. Chang, Tetrahedron 54 (1998) 4413; T. M. Trnka and R. H. Grubbs, Acc. Chem. Res. 2001, 34, 18; S. K. Armstrong, J. Chem. Soc., Perkin Trans. I, 1998, 371; A. Fürstner et al., Chem. Eur. J. 2001, 7, 3236, and the references cited therein). They can be used to form new C—C bonds and thus more complex molecules by simultaneous breaking and formation of unsaturated carbon-carbon bonds, in particular in the presence of selected metal-carbene complexes.

A distinction can be made here between various ring-closing and ring-opening metathesis reaction types. Besides ring-opening metathesis polymerisation (ROMP), which is of no further interest here, (intramolecular) ring-closing metathesis (RCM), cross metathesis (CM) and enyne metathesis (enyne), in particular, are of particular importance. The said metathesis types are illustrated in scheme 1 using the example of a hydrocarbon:

The metathesis reactions are preferably catalyzed by so-called Schrock (or Grubbs) carbene complexes (metal-alkylidene complexes) of transition metals, such as tungsten, molybdenum and in particular ruthenium. These complexes usually have a structure which can be reproduced by the following formula COMP-A (cf., inter alia, WO 96/04289, WO 97/06185, WO 99/00396 and WO 99/00397):

where Met is a transition metal, (L)_(x) stands for a plurality of identical or different ligands, and R_(y) is an organic radical, usually aryl, alkanyl or alkenyl.

The ring-closing metathesis reactions mentioned have also been employed to form heterocyclic ring systems and to prepare corresponding compounds. Thus, nitrogen heterocyclic compounds are accessible in large number by olefin metathesis. According to the literature, oxygen heterocyclic compounds can also be prepared with the aid of this synthetic methodology, but apparently in a significantly smaller structural breadth.

Thus, metathesis processes for the synthesis of pyran derivatives containing both an exocyclic substituent on a carbon atom of the endocyclic C═C double bond formed by metathesis and a 2,5disubstituted

and having industrially useful properties and which can be used, for example, as mesogenic materials or as precursors for the preparation of other compounds having mesogenic properties which contain a pyran ring starting from readily accessible starting compounds have hitherto not been described in the prior art. This is possibly attributable to the fact that the ring-closure reaction to give O-heterocyclic compounds under metathesis conditions has, until the present invention, usually not succeeded or not succeeded reproducibly if one of the carbon atoms of one of the reacting C═C double bonds of the starting compound(s) is disubstituted (cf. also S. K. Armstrong, J. Chem. Soc., Perkin Trans. I, 1998, 371, in particular p. 376).

It is therefore particularly surprising that the ring-closing metathesis starting from compounds of the formula II in the presence of a metathesis catalyst leads reliably and efficiently to the pyran derivatives of the formula I according to the invention.

Preferred metathesis catalysts for the ring-closing metathesis are the transition-metal-alkylidene complexes of the general formula COMP-A described in the prior art (see, inter alia, R. H. Grubbs and S. Chang, Tetrahedron 54 (1998) 4413; T. M. Trnka and R. H. Grubbs, Acc. Chem. Res. 2001, 34, 18; S. K. Armstrong, J. Chem. Soc., Perkin Trans. I, 1998, 371; A. Fürstner et al., Chem. Eur. J. 2001, 7, 3236, and the references cited therein). This is preferably a complex of the formula COMP-A where Met=tungsten, molybdenum or ruthenium. Oxo-tungsten complexes of the trans-W(═O)Cl₂(aryl)₂ type (where aryl is preferably 2,6-dibromophenyl), which have been described, inter alia, by W. A Nugent et al., J. Am. Chem. Soc., 1995, 117, 8992, are furthermore used as metathesis catalysts in the processes according to the invention.

Preferred molybdenum metathesis catalysts are those of the formulae COMP-Mo1, COMP-Mo2, COMP-Mo3 and COMP-Mo4, while the formula COMP-W1 shows a preferred tungsten metathesis catalyst:

Particularly preferred complexes for use as metathesis catalyst in the process according to the invention are ruthenium-alkylidene complexes of the COMP-RuA type, which are known per se from the literature (see, inter alia, WO 96/04289, WO 97/06185, WO 99/00396, WO 99/00397, WO 99/29701, WO 99/51344, WO 00/15339, EP 1 022 282 A2, WO 00/58322, WO 00/71554, WO 02/14336, WO 02/14376, WO 02/083742):

L_(x1) and/or L_(x2) here are preferably anionic ligands, preferably bromine, iodine or in particular chlorine, if desired also e-aralkyl, while Ly and L_(z) are preferably other, usually neutral ligands, such as, for example, PPh₃ (Ph=phenyl), P(i-Pr)₃(i-Pr=isopropyl), PCy₃ (Cy=cyclohexyl), P(Cp)₃ (Cp=cyclopentadienyl), unsubstituted or substituted pyridyl, Im¹, Im² or alkoxy coordinated via the oxygen atom. L_(w) is an optionally present ligand, i.e. w is 0 or 1, where this usually has the same meaning as L_(x1), L_(x2), L_(y) and/or L_(z). R_(z) is an organic radical, in particular aryl, alkanyl or alkenyl.

These ruthenium complexes are generally less sensitive to atmospheric oxygen and tolerate both traces of moisture and also slight impurities. Of the ruthenium-alkylidene complexes COMP-RuA, those of the following formulae COMP-Ru1 to COMP-Ru13 may be mentioned by way of example:

The alkylidene complexes employed as metathesis catalysts are either prepared by processes known from the literature (besides WO 96/04289, WO 97/06185, WO 99/00396, WO 99/00397, WO 99/29701, WO 99/51344, WO 00/1 5339, EP 1 022 282 A², WO 00/58322, WO 00/71554, WO 02/14336, WO 02/14376, WO 02/083742, see, inter alia, also R. H. Grubbs and S. Chang, Tetrahedron 54 (1998) 4413; T. M. Trnka and R. H. Grubbs, Acc. Chem. Res. 2001, 34, 18; S. K. Armstrong, J. Chem. Soc., Perkin Trans. I, 1998, 371; A. Fürstner et al., Chem. Eur. J. 2001, 7, 3236; J. A. Love et al., Angew. Chem. 2002, 114, 4207; K. Grela et al., Angew. Chem. 2002, 114, 4210; G. S. Weatherhead et al., Tetrahedron Lett. 41 (2000) 9553; J. S. Kingsbury et al., J. Am. Chem. Soc. 1999, 121, 791, and the references indicated therein) or are commercially available, for example from SigmaAldrich, Inc. (USA), or Strem Chemicals Inc. (Kehl, Germany).

Some of these catalysts can also be attached to immobilising supports, for example made from polystyrene (for example COMP-Ru3: M. Ahmed et al., Synlett 2000, 1007; or COMP-Ru5a and complexes derived therefrom: St. Randl et al., Synlett 2001, 1547) or glass (for example COMP-Ru5 and complexes derived therefrom: J. S. Kingsbury et al., Angew. Chem. 2001, 113, 4381).

Apart from the above-mentioned molybdenum and tungsten complexes, the catalyst used for the ring-closing metathesis step of the process according to the invention is very particularly preferably a metal complex selected from the group consisting of complexes of the formulae COMP-Ru1, -Ru2, -Ru3, -Ru4, -Ru5, -Ru6, -Ru7, -Ru8, -Ru9, -Ru10, -Ru11, -Ru12 and -Ru13, in particular of the formulae COMP-Ru2a, -Ru3, -Ru5a, -Ru6, -Ru11 and -Ru13. The molar ratio of compound of the formula II to catalyst is generally from 0.001 to 20 mol % (based on the compound of the formula II), preferably from 0.01 to 10 mol %, very particularly preferably from 0.01 to 2 mol % and in particular from 0.01 mol %, to 0.1 mol %.

The ring-closing metathesis of the process according to the invention is carried out under conventional conditions for metal complex-catalyzed reactions of this type. The reaction is carried out without a solvent or in a suitable solvent. The solvent used is an inert solvent, preferably an aromatic and/or halogenated organic solvent and in particular toluene, benzene, chlorobenzene or dichloromethane. The reaction is generally carried out at temperatures from room temperature to the boiling point of the solvent (for example from about 20° C. to 40° C. (dichloromethane) or up to 80° C. or 110° C. (toluene)). The reaction temperature is preferably from 40° C. to 60° C. The reaction time is not crucial per se since the metathesis reaction generally proceeds with complete conversion of the starting material of the formula II and gives the desired pyran derivative of the formula I in good yields. The reaction duration is usually from 10 minutes to 2 days, preferably from 1 hour to 24 hours, in particular from 2 hours to 8 hours.

It is furthermore advantageous to add the catalyst to the reaction mixture in portions, which allows better control of the reaction and results in a reduction in the total amount of catalyst.

In a preferred embodiment of the process according to the invention, compounds of the formula I-A (i.e. compounds of the formula I where W≡C(═O)—) in which Z¹³, Z¹⁴ and Z¹⁵ are not —C(O)— are subjected to a reduction reaction for conversion into a pyran derivative of the formula I in which W is a methylene group (i.e. a pyran derivative of the formula I-B) in a further reaction step after the metathesis reaction step according to the invention. This reduction reaction can be carried out using suitable reducing agents, for example diisobutylaluminium hydride (DIBAH) or boron trifluoride etherate+lithium aluminium hydride or lithium borohydride or sodium borohydride (see J. March: Advanced Organic Chemistry; John Wiley & Sons, New York inter alia, 3rd Edn., 1985, p. 1100, 9-41). Other carboxyl functions (C(═O)O) present in the molecule are also reduced to ether functions (CH₂O) at the same time.

A further preferred embodiment of the process according to the invention includes, as a further reaction step taking place before the ring-closing metathesis step, the reaction of an acrylic compound or allyl compound of the formula IV with a homoallyl compound of the formula V with formation of the compound of the formula II

where X¹¹ is a leaving group, and a, b, c, d, e, W. R¹¹, R¹², Z¹¹, Z¹², Z¹³, Z¹⁴, Z¹⁵, A¹¹, A¹², A¹³, A¹⁴ and A¹⁵ in the formulae II, IV and V are as defined for the formula I above.

If W is —C(═O)— (i.e. the compound of the formula IV is an acrylic derivative (formula IV-A)), X¹¹ is preferably methoxy, ethoxy, propoxy, t-butoxy, chlorine, bromine or an anhydride radical, in particular acetoxy. The process step then proceeds under the usual conditions for ester formation reactions of this type (cf., inter alia, J. March: Advanced Organic Chemistry; John Wiley & Sons, New York inter alia, 3rd Edn., 1985, pp. 346-351, 0-22, 0-23 and 0-24).

W is preferably —CH₂— (i.e. the compound of the formula IV is an allyl derivative (formula IV-B)). In this case, X¹¹ is preferably chlorine, bromine, iodine or a sulfonic acid radical, for example CF₃—SO₃—, CH₃—SO₃—, C₄F₉—SO₃— or p-CH₃—C₆H₄—SO₃—. The ether formation reaction step according to the invention is generally carried out under the conditions of the Williamson ether synthesis (see, for example, J. March: Advanced Organic Chemistry; John Wiley & Sons, New York inter alia, 3rd Edn., 1985, p. 342, 0-14), i.e. under basic reaction conditions and at temperatures from room temperature to about 60° C. in suitable solvents, for example ethers, such as tetrahydrofuran (THF), methyl tert-butyl ether (MTBE), dioxane or dimethoxyethane. A particularly preferred variant of this reaction works with granulated NaOH in THF in the presence of a phase-transfer catalyst and a little water, with the allyl compound of the formula IV-B where X¹¹=bromine or chlorine and the homoallyl alcohol of the formula V being warmed at from 40° C. to 60° C. for from 4 to 48 hours. This variant is particularly suitable for homoallyl alcohols of the formula V which do not contain a carboxyl function (i.e. homoallyl alcohols of the formula V in which Z¹³, Z¹⁴ and Z¹⁵ are not CO₂). Alternatively, the base employed can be sodium hydride, preferably in an organic solvent.

The acrylic compounds or allyl compounds of the formula IV and homoallyl compounds of the formula V employed in the process according to the invention are—if they are known from the literature—either commercially available or are prepared by methods known per se, as described in the literature (for example the standard works, such as Houben-Weyl, Methoden der Organischen Chemie [Methods of Organic Chemistry], Georg-Thieme-Verlag, Stuttgart), to be precise under reaction conditions which are known and suitable for the reactions mentioned therein. Use can also be made here of variants which are known per se, but are not mentioned here in greater detail.

The allyl compounds of the formula IV-Ba where a=b=0 can be obtained, inter alia, via the allyl alcohols of the formula IV-Ba1, which are accessible in accordance with a Weigand and BrOckner process (S. Weigand, R. Brückner, Synthesis 1996, 475) as shown in scheme 2. The conversion of formula IV-Ba1 into the allyl compounds of the formula IV-Ba2 is carried out by known processes, for example using bromine/triphenylphosphine for X¹¹=Br and by means of trifluoromethanesulfonyl chloride or trifluoromethanesulfonic anhydride for X¹¹=CF₃SO₃.

The synthesis of the allyl derivatives of the formula IV-Bb where a and/or b are 1, which were hitherto unknown, is carried out analogously and is shown in scheme 3:

Instead of the substituted malonic acid diesters Vo-IVa or VoIVb, the allyl derivatives of the formula IV-B can also be prepared using the corresponding diols of the formula Vo-IVc, which are known from the literature or are accessible analogously to known processes (see, inter alia, P. Kirsch and E. Poetsch, Adv. Mater. 1998, 10, 602, and the references indicated therein; C. Tschierske et al., Mol. Cryst. Liq. Cryst. 1990, 191, 295; EP 400 846 A1). The precursor Vo-IVc gives, for example after dihalogenation and treatment with 1 equivalent of potassium tert-butoxide, the allyl compound IV-B where X¹¹=halogen.

The allyl alcohols of the formulae IV-Ba1 and IV-Ba2 are also accessible analogously to a process of H. Mitzutani et al. (Tetrahedron 58 (2002) 8929) from the corresponding acrolein derivatives with NaBH₄/CeCl₃; the acrolein derivatives are themselves obtained from the corresponding aldehyde R¹¹-Z¹²-CH₂—CHO or R¹¹-[-A¹¹]_(a)-[-Z¹¹-A¹²-]_(b)-Z¹²-CH₂—CHO using Eschenmoser's reagent.

The novel allyl derivatives of the formula IV-Bb

where

-   a is zero and b is 1 or a is 1 and b is zero or a and b are both 1; -   X^(11a) is chlorine, bromine, iodine, a sulfonic acid radical, —OH,     alkoxy or O-aralkyl, or X^(11a) is ═O; -   R¹¹, Z¹¹ and Z¹² are as defined for the formula I above; and -   A¹¹ and A¹² are as defined for the formula I above and are     preferably 1,4-cyclohexylene;     are likewise a subject-matter of the present invention as useful     intermediates for the preparation of the compounds of the formula I     according to the invention. They are prepared as described above and     in the attached examples; the compounds of the formula IV-Bb where     X^(11a)=alkoxy or O-aralkyl are accessible, inter alia, by reaction     of the corresponding compounds of the formula IV-Bb where     X^(11a)=Cl, Br, I or a sulfonic acid radical with a corresponding     alcohol (alkyl-O—H or aralkyl-O—H). The aldehydes of the formula     IV-Bb (where -X^(11a) is ═O) according to the invention are also     accessible from the allyl alcohols of the formula IV-Bb (where     X^(11a) is —OH) by mild oxidation using, for example, manganese     dioxide.

The corresponding acrylic derivatives of the formula IV-A are accessible, inter alia, by oxidation of the corresponding allyl alcohols of the formula IV-Ba1 or IV-Bb1 using a strong oxidant, such as a chromium(VI) oxidant (J. March: Advanced Organic Chemistry; John Wiley & Sons, New York inter alia, 3rd Edn., 1985, p. 1084, 9-22). Alternatively, the allyl alcohols may also firstly be converted into the corresponding aldehydes (acrolein derivatives) using a relatively mild oxidant, such as manganese dioxide (MnO₂), which are then converted into the acrylic derivatives of the formula IV-A, for example using an alkaline Ag₂O or silver nitrate solution or by means of atmospheric oxygen.

The homoallyl compounds of the formula V are accessible as shown in scheme 4 by reaction of aldehydes of the formula Vo-Va with allyl bromide (it also being possible to use other allyl halides, in particular allyl chloride, instead of the bromide):

The requisite activation of the allyl halide can be carried out in various ways: for example, addition of allyl bromide to indium powder in a suitable reaction medium, for example water or water/tetrahydrofuran, firstly forms a corresponding intermediate allylindium compound (by the method of T.-P. Loh et al., Tetrahedron Letters 42 (2001) 8701 and 8705) which then reacts with the aldehyde Vo-Va with formation of the corresponding homoallyl alcohol V. Allyl bromide can also be converted into the corresponding intermediate allyllithium or allylmagnesium bromide compound using lithium or an organolithium base or using magnesium, usually in excess, or a reactive Grignard base with halogen-metal exchange, and this intermediate then reacts with the aldehyde Vo-Va to give the homoallyl alcohol V. If the aldehyde Vo-Va additionally contains an ester or nitrile function, it is advantageous to transmetallate the intermediate allyllithium or allylmagnesium bromide compound in a known manner using zinc or titanium salts, since the corresponding allylzinc or allyltitanium compounds only react chemoselectively with the aldehydic carbonyl function and not with the ester carboxyl or the nitrile function.

It is furthermore also possible to employ allyl derivatives of other metals and semimetals, for example allyl derivatives of chromium, tin, zinc, samarium, boron and silicon, for the preparation of the homoallyl compounds V. Starting from allyl mesylate (bromine in allyl bromide is replaced by a mesylate radical (—OSO₂CH₃)), the corresponding allyl stannanes are accessible by transmetallation using, for example, LiSn(butyl)₃, and can also be prepared by reaction of allyl bromide with tin(II) chloride and potassium iodide in water (cf. V. V. Samoshin et al., Tetrahedron Lett. 43 (2002) 6329) or with tin metal under the action of ultrasound and water (cf. P. C. Andrews, Tetrahedron Lett. 43 (2002) 7541) and can be reacted with the aldehyde Vo-V to give the homoallyl alcohol V.

Correspondingly, the allylzinc compound is obtainable, inter alia, using zinc dust in tetrahydrofuran (cf. B. C. Ranu et al., Tetrahedron Lett. 36 (1995), 4885), the allylsamarium compound is obtainable using Sml₂ in tetrahydrofuran (cf. B. Hamann-Gaudinet et al., Tetrahedron Lett. 38 (1997) 6585) or the allylchromium compound, which can be reacted with an aldehyde Vo-V to give homoallyl alcohols V, is obtainable using Cr(II)Cl₂/Mn.

Since the aldehydes of the formula Vo-V have a prochiral center on the carbonyl carbon atom, a center of chirality is formed on the carbon atom carrying the hydroxyl function in the reaction with the activated allyl derivative formed from allyl bromide to give the homoallyl alcohol V. In general, a racemate of the optical antipodes of the homoallyl alcohol V forms in the process. However, it is also possible to prepare one of the optical isomers of the homoallyl alcohol V stereoselectively or alternatively to isolate it from the racemic mixture.

The stereoselective synthesis is preferably carried out by catalytic asymmetric allylation of the aldehyde of the formula Vo-V using an allyltin compound, usually allyltributylstannane, in the presence of a chiral catalyst. Suitable chiral catalysts are, in particular, complexes of chiral binaphthol (BINOL) compounds with zirconium (for example (R,R)- or (S,S)-BINOL-Zr(O-tert-butyl)₄: M. Kurosu et al., Tetrahedron Lett. 43 (2002) 1765) or titanium (for example bis(((S)(naphthoxy)(isopropoxy)titanium oxide: H. Hanawa et al., J. Am. Chem. Soc. 2003, 125, 1708) or corresponding boronates (cf., for example, S. Thormeier et al., J. Organomet. Chem. 657 (2002) 136). In principle, the R- or S-isomer is accessible selectively in this way—depending on the choice of the chiral catalyst.

The enantiomers are isolated from the racemic mixture by conventional methods, for example by crystallization with a chiral base or chromatography on a chiral column material.

Through use of an enantiomerically pure homoallyl alcohol of the formula V accessible in this way, the corresponding pyran derivative of the formula I, which has a center of asymmetry in the 2-position, is obtained in enantiomerically pure form via the intermediate II after the ring-closing metathesis reaction according to the invention. A further possibility for obtaining one of the optical antipodes of the pyran derivative of the formula I stereoselectively consists in the use of a chiral metathesis catalyst, for example COMP-Mo3 or COMP-Mo4 (G. S. Weatherhead et al., Tetrahedron Lett. 41 (2000) 9553).

Aldehydes of the formula Vo-Va are known as such from the literature (see, inter alia, EP 0 122 389 A2) or can be prepared analogously thereto. Aldehydes of the formula Vo-Va where Z¹³=CF₂O are synthesised, for example, starting from the acid chloride ethyl-O—C(═O)—C(═O)—Cl  Vo-Vb by reaction with firstly NaS-(CH₂)₃—SH. The resultant thiol thioester is reacted with trifluoromethanesulfonic acid (analogously to the processes described by P. Kirsch et al., Angew. Chem. 2001, 113, 1528, and WO 01/64667) to give the corresponding bis(alkylthio)carbenium salt

which is then subjected to oxidative fluorodesulfuration (as described by P. Kirsch et al., Angew. Chem. 2001, 113,1528, and WO 01/64667) by reacting the bis(alkylthio)carbenium salt of the formula Vo-Vc firstly at low temperatures with NEt₃·3 HF (Et=ethyl) and an alcohol of the formula HO—[A¹³-Z¹⁴]_(c)-[A¹⁴-Z¹⁵]_(d)-[A¹⁵]_(e)—R¹²  Vo-Vd, then with 1,3-dibromo-5,5-dimethylhydantoin (DBH) or N-bromosuccinimide (NBS) or bromine and finally with aqueous caustic lye to give the ester ethyl-O—C(═O)—CF₂O—[A¹³-Z¹⁴]_(c)-[A¹⁴-Z¹⁵]_(d)-[A¹⁵]_(e)—R¹²  Vo-Ve.

The final introduction of the aldehyde function to give the aldehyde of the formula Vo-Va is carried out either by direct reduction of the ester using a suitable reducing agent, such as diisobutylaluminium hydride, in an inert solvent, for example methylene chloride, or via reduction of the ester to give the corresponding alcohol and subsequent oxidation to the aldehyde using a suitable oxidant, for example Dess-Martin reagent.

An alternative synthetic route which is suitable, in particular, for the preparation of aldehydes of the formula Vo-Va in which the difluorooxymethylene bridge is linked to an aromatic radical starts from the ester ethyl-O—C(═O)—CF₂Br, which is converted into the desired aldehyde Vo-Va using a suitable phenoxide in the presence of, for example, hexamethylenephosphoric tribromide or with Pd⁰ complex catalysis with formation of the CF₂O bridge and after final reduction of the ester function.

If the aldehyde of the formula V-IV is a phenanthrene derivative of the formula

this is accessible in accordance with scheme 5 below:

In step (1), C—C coupling is carried out with Pd⁰ catalysis to give the biphenyl, which is converted into the divinyl derivative in step (2) using vinylmagnesium bromide or vinylzinc bromide in the presence of a palladium complex (PdCl₂. bis-(diphenylphosphino)ferrocene). In step (3), an intramolecular cross metathesis to give the phenanthrene derivative is carried out in the presence of a ruthenium-alkylidene complex COMP-RuA, preferably COMP-Ru2a-c or COMP-Ru4. The chlorophenanthrene is subsequently converted into the ethyl ester in step (4) using CO/ethanol at 70° C. and 5 bar in the presence of PdCl₂·[2P(cyclohexyl)₃] as catalyst, and this ethyl ester gives the desired phenanthrene aldehyde after final reduction using DIBAH in step (5).

For the preparation of the phenanthrene aldehyde of the formula

the chlorine-substituted compound in step (1) of scheme 5 is replaced by the corresponding benzyloxy compound

which is correspondingly converted into the corresponding benzyloxy-substituted phenanthrene compound in steps (1) to (4). After reductive removal of the benzyloxy protecting group (using hydrogen and Pd/C), the resultant hydroxyphenanthrene is converted into the desired aldehyde as described above using ethyl-O—C(═O)—CF₂Br and after final reduction of the ester function. The starting compounds for these phenanthrene syntheses are either commercially available or readily accessible by known synthetic methods.

The starting compounds necessary for the preparation of compounds of the formula I-G according to the invention by the process according to the invention by ring-closing metathesis reaction are also accessible by a further process which is illustrated in scheme 6:

In this process, firstly the acid VII is prepared, for example, from the allyl alcohol IV and bromoacetic acid VI (as described, for example, in J. March: Advanced Organic Chemistry; John Wiley & Sons, New York inter alia, 3rd Edn., 1985, p. 342, 0-14), and subsequently converted into the compound VIII using allyl alcohol under conventional conditions (cf., inter alia, J. March: Advanced Organic Chemistry; John Wiley & Sons, New York inter alia, 3rd Edn., 1985, pp. 346-351, 0-22, 0-23 and 0-24).

This is subsequently subjected to a Claisen rearrangement (see, for example, J. March: Advanced Organic Chemistry; John Wiley & Sons, New York inter alia, 3rd Edn., 1985, p. 1028, 8-37), for example by firstly adding lithium diisopropylamide (LDA) and then a 1:1 mixture of trimethylsilyl chloride and triethylamine to a solution of VIII in THF at very low temperatures (about −100° C.), slowly thawing the mixture, adding aqueous base or acid, and subjecting the mixture to conventional work-up to give the acid II-1. The ring-closing metathesis reaction according to the invention is preferably carried out using an ester II-2 instead of the free carboxylic acid II-1, this ester being prepared by conventional esterification methods and giving, after the metathesis reaction, the compounds of the formula I-G according to the invention.

It goes without saying that firstly precursors and starting compounds of the formulae II, IV and V for compounds of the formula I according to the invention can be prepared from other suitable precursors and starting compounds of the formulae II, IV and V, and secondly compounds of the formula I according to the invention can also be converted, after the ring closure, into other pyran derivatives of the formula I according to the invention. Carboxylic acid, benzyloxy and halogen derivatives have proven particularly useful here.

Thus, for example, the carboxylic acid ester of the formula II-2 (where c=d=e=0 and R¹² is aralkyl, alkanyl or alkenyl) can firstly be subjected to a ring-closing metathesis reaction with formation of the corresponding pyran derivative of the formula I-G (where c=d=e=0 and R¹² is aralkyl, alkanyl or alkenyl). Transesterification of this ester with synthetic units of the HO-[A¹³-Z¹⁴]_(c)-[A¹⁴-Z¹⁵]_(d)-[A¹⁵]_(e)-R¹² type then enables other compounds of the formula I-G according to the invention to be obtained. However, a corresponding esterification can also, if desired, be carried out with precursor II-1 before the ring-closing metathesis reaction.

The carboxylic acids of the formula I-G according to the invention (where R¹²=H and c=d=e=0), which are prepared from the corresponding esters by basic or acidic saponification, can be employed in order to obtain the corresponding CF₂O-bridged pyran derivative of the formula I-H via the corresponding bis(alkylthio)carbenium salt followed by oxidative fluorodesulfuration (cf. WO 01/64667). The oxidative fluorodesulfuration can of course also be used for compounds of the formula I according to the invention in which the carboxyl function is not linked directly to the central pyran ring, i.e. if Z¹⁴ or Z¹⁵=—CO₂H; in this way, —CF₂O-[A¹⁴-Z¹⁵]_(d)-[A¹⁵]_(e)-R¹²- or —CF₂O-A¹⁵-R¹²-radicals respectively are then introduced.

Aldehydes of the formula I according to the invention where Z¹³-R¹²═—C(═O)—H are accessible from the carboxylic acid esters of the formula I-G according to the invention where R¹²≈ H and c=d=e=0 either by direct reduction, for example using a suitable metal hydride, or in two steps by reduction to the primary alcohol followed by gentle oxidation using, for example, Dess-Martin reagent. The reduction to pyran derivatives according to the invention containing an aldehyde function can of course also be carried out with compounds of the formula I in which the carboxylic acid ester function is not linked directly to the central pyran ring, i.e. if Z¹⁴ or Z¹⁵=—CO₂R¹². In this way, the —C(═O)—H function is introduced as radical Z¹⁴-R¹² or Z¹⁵-R¹².

The corresponding compounds of the formula I according to the invention where Z¹³, Z¹⁴ or Z¹⁵=-CH═CH— are accessible from the aldehydes of the formula I accessible in this way, for example by means of a Wittig or Wittig-Horner reaction with molecules of the R^(x)-[A¹³-Z¹⁴]_(c)-[A¹⁴-Z¹⁵]_(d)-[A¹⁵]_(e)-R¹² type (where R^(x) is, for example, (phenyl)₃P═CH— or (ethyl-O)₂P(═O)—CH₂—).

The ketones of the formula I according to the invention where Z¹³-R¹², Z¹⁴-R¹² or Z¹⁵-R¹²═—C(O)—R¹² and R¹²=alkanyl, alkenyl or aralkyl are prepared, for example, by reaction of the corresponding carboxylic acid ester of the formula I-G with a suitable organometallic reagent, for example with a compound R¹²-Mg-Br by the Grignard method (see, for example, J. March: Advanced Organic Chemistry, John Wiley & Sons, New York inter alia, 3rd Edn., 1985, p. 434, 0-107). Further ketones of the formula I where, for example, Z¹³-[A¹³-Z¹⁴]_(c)-[A¹³-Z¹⁵]_(d)-[A¹⁵]_(e)-R¹² is —C(O)-[A¹³-Z¹⁴]_(c)-[A¹⁴-Z¹⁵]_(d)-[A¹⁵]_(e)-R¹² are also accessible analogously by reaction with a suitable organometallic reagent Met*-[A¹³-Z¹⁴]_(c)-[A¹⁴-Z¹⁵]_(d)-[A¹⁵]_(e)-R¹² (where “Met*” is, for example, Br—Mg or Li). If Z¹⁴ and Z¹⁵ are not CO₂ and R¹² does not contain a carboxyl function, the ketones of the formula I are obtainable by reduction of the corresponding esters of the formula I-G. Keto functions can also be introduced analogously as Z¹⁴ or Z¹⁵.

Compounds of the formula I-K according to the invention are also highly suitable for further derivatisations. Reaction on the cyclohexanone ring with, for example, trimethylsilyl-1,3-dithiane in THF in the presence of n-butyllithium (in accordance with the method of J. Mlynarski and A. Banaszek, Tetrahedron 55 (1999) 2785) or analogously to the processes of P. Kirsch et al., Angew. Chem. 2001, 113, 1528, gives the corresponding ketene dithioketals (containing the structural unit

Oxidative fluorodesulfuration (by the method of P. Kirsch et al., Angew. Chem. 2001, 113, 1528) then gives compounds of the formula I according to the invention containing

as structural unit.

The cyclohexanones of the formula I-K according to the invention can also be reacted with a suitable Grignard reagent, for example of the Br—Mg-Z¹⁴-A¹⁴-R¹² type where Z¹⁴ is, for example, —CH₂— or —CH₂CH₂—, to give the corresponding tertiary alcohols, in this example containing the structural unit

Subsequent reduction of the alcohol using triethylsilane and boron trifluoride etherate gives the corresponding 1,4-disubstituted cyclohexane derivative (in the example mentioned containing the structural unit

Compounds of the formula I according to the invention which contain a terminal phenyl ring where R¹²=halogen, in particular bromine or iodine, for example corresponding compounds of the formula I-CBI, I-CBII, I-CBIIIc, I-GII, I-GIll, I-HI, I-HII or I-J, can likewise be employed as starting compounds for the preparation of further compounds of the formula I according to the invention. Thus—after metallation with metal-halogen exchange, for example using an organometallic base, such as n-butyl-lithium—the intermediate metallated compound can be reacted further with various reagents, for example with CO₂ with formation of the corresponding carboxylic acid, with boric acid esters or related boron compounds with formation of the corresponding arylboron compounds, or in the presence of suitable catalysts with reactants which undergo C—C cross-coupling reactions, for example of the Heck or Suzuki reaction type.

The said arylboron compounds or the halogenated compounds themselves can also be reacted in cross-coupling reactions of this type which are known from the literature (see, for example, N. Miyaura, A. Suzuki, Chem. Rev. 1995, 95, 2457). It should furthermore be noted that certain precursors and starting compounds of the processes according to the invention, for example those in which an aromatic ring A¹³ is linked directly to an aromatic ring A¹⁴ (or A¹⁵) via Z¹⁴ (or Z¹⁵)=single bond, can also be prepared with the aid of these cross-coupling reactions.

It is furthermore preferred in the process according to the invention, after the ring-closing metathesis reaction step, to carry out, as a further reaction step, a catalytic hydrogenation to give a pyran derivative of the general formula III:

in which

-   f, g, h, j and k are each, independently of one another, 0 or 1; -   R³¹ is H, an alkyl radical having from 1 to 15 carbon atoms which is     unsubstituted or mono- or polysubstituted, identically or     differently, by halogen or —CN, where, in addition, one or more CH₂     groups in this radical may be replaced by —O—, —S—, —C(O)—O and/or     —O—C(O)— in such a way that hetero atoms (O and S) are not linked     directly to one another; -   R³² is H, halogen, —CN, —NCS, aralkyl or an alkyl radical having     from 1 to 15 carbon atoms which is unsubstituted or mono- or     polysubstituted, identically or differently, by halogen or —CN,     where, in addition, one or more CH₂ groups in this radical may be     replaced by —O—, —S—, —C(O)—O— and/or —O—C(O)— in such a way that     hetero atoms (O and S) are not linked directly to one another; -   Z³¹ and Z³², independently of one another, are a single bond, —CH₂—,     —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂— or —CF₂CF₂—; -   Z³³, Z³⁴ and Z³⁵ are each, independently of one another, a single     bond, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂—, —CF₂CF₂—, —CH₂O—, —CF₂O—, —C(O)—     or —C(O)—O—; -   A³¹ and A³², independently of one another, are -   A³³ and A³⁴, independently of one another, are -   A³⁵ is -   A³⁵-R³² together are     or -   Z³³-[-A³³-Z³⁴-]_(h)-[-A³⁴-Z³⁵-]_(j)-[-A³⁵-]_(k)—R³² is     where R³² is as defined above, and L³⁷, L³⁸ and L³⁹, independently     of one another, are H or F; -   r is 0, 1, 2, 3 or 4; -   s is 0, 1, 2 or 3; -   R³³ and R³⁴, independently of one another, are an alkanyl radical     having from 1 to 7 carbon atoms or together are an alkylene bridge     having from 2 to 7 carbon atoms;     with the proviso that, in the case of direct linking of Z³³ and R³²     to give -Z³³-R³², R³² is H, aralkyl or alkanyl if Z³³ is —C(═O)—,     R³² is aralkyl or alkanyl if Z³³ is —C(═O)—O—, and Z³³ is not —CH₂O—     or —CF₂O—; that, in the case of direct linking of Z³⁴ and R³² to     give -Z³⁴-R³², R³² is H, aralkyl or alkanyl if Z³⁵ is —C(═O)—, R³²     is aralkyl or alkanyl if Z³⁴ is —C(═O)—O—, and Z³⁴ is not —CH₂O— or     —CF₂O—; that, in the case of direct linking of Z³⁵ and R³² to give     -Z³⁵-R³², R³² is H, aralkyl or alkanyl if Z³⁵ is —C(═O)—, R³² is     aralkyl or alkanyl if Z³⁵ is —C(═O)—O—, and Z³⁵ is not —CH₂O— or     —CF₂O—; that R³¹ is not H if simultaneously f and g are both zero     and Z³² is a single bond.

Starting compounds which can be employed for the preparation of a pyran derivative of the general formula III are in principle all compounds of the formula I according to the invention where W≡CH₂—(i.e. compounds of the formula I-B). Besides the (endocyclic) C═C double bond in the central pyran ring, further aliphatic C═C double bonds optionally present in the compound of the formula I-B are also hydrogenated to a C—C single bond during the hydrogenation. Thus, for example, catalytic hydrogenation of a compound of the formula I-CB gives the corresponding compound of the formula III-CB (see scheme 7), where the meaning of f, g, h, j, k, R³¹, R³², Z³¹, Z³³, Z³⁴, Z³⁵, A³¹, A³², A³³, A³⁴ and A³⁵ in the formula III-CB corresponds to the meaning of a, b, c, d, e, R¹¹, R¹², Z¹¹, Z¹³, Z¹⁴, Z¹⁵, A¹¹, A¹², A¹³, A¹⁴ and A¹⁵ respectively in the formula I-CB and Z¹²=Z³²=single bond, with the proviso that, if Z¹¹, Z¹³, Z¹⁴ and/or Z¹⁵ are —CH═CH— or R¹¹ and/or R¹² contain a —CH═CH— group, these aliphatic —CH═CH— groups are converted into CH₂—CH₂ groups.

Analogously, the compounds of the formula I-DB according to the invention give the corresponding hydrogenated compounds III-DB, I-EB give III-EB, I-FB give III-FB, I-GB give III-GB, I-JB give III-JB, I-KB give III-KB, I-LB give III-LB, I-MB give III-MB, I-NB give III-NB, I-OB give III-OB, I-PB give III-PB, I-QB give III-QB, I-RB give III-RB, I-SB give III-SB and I-TB give III-TB. Illustrative compounds of the formula III are those which are derived from the pyran derivatives of the formula I shown in Tables 1 to 6 and differ therefrom in that they do not contain a C═C double bond in the central pyran ring. (For simplicity and better congruence, compounds of the formula III are also referred to as compounds of the formula III-B).

The catalytic hydrogenation is usually carried out at a hydrogen partial pressure of from 1 bar to 10 bar. The hydrogenation catalysts employed are usually transition-metal catalysts comprising nickel, platinum or palladium, such as, for example, Raney nickel, 5% or 10% platinum on carbon and 5% palladium on activated carbon, in a suitable solvent, such as, for example, n-heptane, ethyl acetate, toluene, ethanol, methanol or THF. The reaction time is not crucial per se; the hydrogenation is usually carried out to complete conversion of the respective starting compound. The reaction temperature is generally in the range between room temperature and 100° C.

In the hydrogenation of the pyran derivative I to the pyran derivative III, a further chiral center is formed in the 5-position in addition to the center of asymmetry in the 2-position of the pyran ring. If the starting compound employed for the catalytic hydrogenation for formation of the tetrahydropyran III is a pyran derivative of the formula I which, after corresponding stereoselective synthesis described above or purification, is in enantiomerically pure (or enantiomerically enriched) form, only 2 of the 4 theoretically conceivable diastereomers of III are usually obtained (depending on the absolute configuration on the C-2 atom having the 2R,5R- and 2R,5S- or 2S,5R- and 2S,5S-configuration). These two isomers, which behave as diastereomers to one another, can be separated from one another by conventional methods, such as fractional crystallization or chromatography, enabling the tetrahydropyran of the formula III also to be obtained in enantiomerically pure form. The isomerically pure compounds of the formula III, like the isomerically pure compounds of the formula I, are used, inter alia, as chiral dopants for nematic liquid-crystalline media which effect the twisted arrangement of the compounds present in the liquid-crystalline media which is necessary for various electro-optical applications.

It is of course possible for compounds of the formula III themselves to be converted into other compounds of the formula III, by means of the same synthetic processes explained in detail above for the compounds of the formula I according to the invention. As also in the case of the compounds of the formula I according to the invention which contain a carboxyl function, carboxylic acid esters of the formula III-GB, in particular those of the formula III-GBI, are particularly suitable for this purpose. They can be saponified, for example, to give the corresponding free carboxylic acid, debenzylated by hydrogenation or desallylated with palladium catalysis and then further derivatised in order to facilitate, for example, the introduction of a difluorooxymethylene bridge. Of many other derivatisation possibilities, mention should also be made here by way of example of the possibility of reducing the ester of the formula III-GBI to the corresponding aldehyde, which can itself be reacted in a Wittig or Wittig-Horner reaction with introduction of an aliphatic C═C double bond.

Furthermore, the compounds of the formula III-KB are not only accessible directly by hydrogenation of corresponding compounds of the formula I-KB. They can also, for example, be prepared by firstly hydrogenating a pyran derivative of the formula I-B containing a terminal phenyl ring where R¹²=O-aralkyl, such as, for example, compounds of the formula I-CBIIa where R^(12a)=aralkyl, with simultaneous debenzylation to give the corresponding compound of the formula III-B containing a terminal phenol ring, and subsequently converting the product into the corresponding compound of the formula III-KB containing a terminal cyclohexanone ring using suitable reducing agents (see, for example, J. March: Advanced Organic Chemistry; John Wiley & Sons, New York inter alia, 3rd Edn., 1985, p. 700, 5-11). For the illustrative compounds, this procedure is shown by scheme 8. The compounds of the formula III-KB are particularly suitable for the introduction of CF₂O bridges, the details of which are described above for the reaction of the cyclohexanone derivatives of the formula I-KB, which are likewise in accordance with the invention.

Owing to the 2,5-disubstitution of the central pyran ring, the compound of the formula III can be in the form of either the cis- or the trans isomer. The trans isomer, which is generally preferred for many uses, is occasionally obtained as the only hydrogenation product. If the pyran of the formula III is formed predominantly as the cis isomer or as a mixture of the two isomers, the preferred trans isomer is obtained from the cis isomer by treatment with a strong base, for example potassium tert-butoxide in N-methylpyrrolidone, or with a strong acid, for example sulfuric acid in dioxane.

The compounds of the formula III are mesogenic, preferably liquid-crystalline, and are used in liquid-crystalline media.

The present invention furthermore relates to the use of a pyran derivative of the above formula I or of the formula III as constituent of a liquid-crystalline medium which is employed, in particular, in electro-optical display devices, such as TN, STN and active-matrix displays. These electro-optical display devices are, for example, displays of mobile radio equipment, screens of portable computers (notebooks) and TFT flat-panel screens.

The abbreviation m.p. denotes melting point, and cl.p. denotes clearing point. Furthermore, C=crystalline state, N=nematic phase, S=smectic phase and I=isotropic phase. S_(C) denotes a smectic C phase, S_(B) a smectic B phase, S_(A) a smectic A phase. Δn denotes the optical anisotropy (Δn=n_(e)−n_(o), where n_(e) denotes the refractive index of the extraordinary ray and n_(o) denotes the refractive index of the ordinary ray) (589 nm, 20° C.). Δε denotes the dielectric anisotropy (Δε=ε_(∥)-ε_(⊥), where ε_(∥) denotes the dielectric constant parallel to the longitudinal molecular axes, and ε_(⊥) denotes the dielectric constant perpendicular thereto) (1 kHz, 20° C.). The optical data are measured at 20° C., unless expressly stated otherwise. The rotational viscosity γ₁[mPa·s] is likewise determined at 20° C. The physical parameters are determined experimentally as described in “Licristal, Physical Properties Of Liquid Crystals, Description of the measurement methods”, Ed. W. Becker, Merck KGaA, Darmstadt, revised edition, 1998, with the properties of individual compounds in some cases being determined after measurement of a defined amount of the compound (usually 5 or 10% by weight) in a defined host mixture having known properties followed by extrapolation.

Without further elaboration, it is believed that one skilled in the art can, using the preceding description, utilize the present invention to its fullest extent. The following preferred specific embodiments are, therefore, to be construed as merely illustrative, and not limitative of the remainder of the disclosure in any way whatsoever.

In the foregoing and in the following examples, all temperatures are set forth uncorrected in degrees Celsius and, all parts and percentages are by weight, unless otherwise indicated.

EXAMPLES

The starting compounds, reagents and solvents employed in the illustrative syntheses are either purchased or prepared by processes known from the literature. The illustrative syntheses are usually carried out in dry apparatuses with exclusion of moisture and—if required by the reaction in question—also under a protective-gas atmosphere for exclusion of air.

The course of reactions is generally monitored by thin-layer chromatography or gas chromatography. The reaction products are worked up and purified by conventional methods, for example by column chromatography or crystallization. Their structural identity is ensured by mass spectrometry and ¹H-NMR spectroscopy. The yields are not optimized.

Example 1 Ring-Closing Metathesis

General Working Procedure B1 (GWP B1)

Compound B 1.1 (100 mmol), as a solid or dissolved in toluene, is warmed to from 40 to 60° C. under a nitrogen atmosphere. Tricyclohexylphosphine-(1,3-bis(2,4,6-trimethylphenyl)-4,5-dihydroimidazol-2-ylidenebenzylideneruthenium dichloride (COMP-Ru2a) (from 0.1 to 0.5 mmol; Strem Chemicals Inc., Kehl, Germany) is then added in one portion, whereupon very vigorous gas evolution immediately commences. The mixture is stirred at 60° C. for 15 minutes. After the gas evolution due to the ethene formed by the reaction has subsided, some more catalyst (0.05-0.1 mmol) is added in order to ensure the end of the reaction due to the continuing foaming. The reaction mixture is purified on silica gel, giving product B 1.2 after crystallization or vacuum distillation. Yields: 45-75%.

Some of the compounds prepared as described in GWP B1 are shown in Table B1.

(If the reaction is carried out on a larger scale, the catalyst is added in portions (usually from 4 to 8 portions of about 0.0025 mol % each). The end of the reaction is indicated by gas evolution no longer being observed after repeated addition of catalyst). TABLE B1 Compound B 1.2 No. R^(B1) R^(B2) -1

-2

-3

-4 n-C₃H₇

-5 n-C₃H₇

-6

-7

-8 CH₃

-9 CH₃

-10 CH₃

-11

-12

-13 C₂H₅

-14 n-C₃H₇

-15 n-C₃H₇

-16 C₂H₅

-17 C₂H₅

-18 n-C₃H₇

-19 n-C₃H₇

-20 n-C₃H₇

-21 C₂H₅

-22 n-C₃H₇

-23 n-C₅H₁₁

-24 n-C₃H₇

-25 n-C₃H₇

-26 n-C₃H₇

-27 n-C₃H₇

-28 n-C₄H₉

-29 n-C₄H₉

-30 n-C₃H₇

-31 n-C₃H₇

-32 C₂H₅

-33 n-C₃H₇

-34 n-C₃H₇

-35 n-C₃H₇

-36 n-C₃H₇

-37 C₂H₅

-38 C₂H₅

-39 C₂H₅

-40 n-C₃H₇

-41 C₂H₅

-42 C₂H₅

-43 n-C₃H₇

-44 n-C₃H₇

-45 n-C₃H₇

-46 n-C₃H₇

-47 n-C₃H₇

-48 n-C₃H₇

-49 C₂H₅

-50 C₂H₅

-51 C₂H₅

-52 n-C₃H₇

-53 n-C₃H₇

-54 n-C₃H₇

-55 n-C₃H₇

-56 n-C₃H₇

-57

-58 n-C₃H₇

-59 n-C₃H₇

-60 n-C₃H₇

-61 n-C₃H₇

-62 CH₃

-63

-64 n-C₃H₇

-65 n-C₃H₇

-66

-67 n-C₃H₇

-68 n-C₃H₇

-69 n-C₅H₁₁

-70 C₂H₅

-71 C₂H₅

-72 n-C₄H₉

-73 n-C₃H₇

-74 n-C₃H₇

-75 C₂H₅

-76 C₂H₅

-77 n-C₅H₁₁

-78 n-C₄H₉

-79 n-C₇H₁₅

-80 n-C₄H₉

-81 n-C₅H₁₁

-82 n-C₇H₁₃

-83 CH₃

-84 n-C₄H₉

-85 n-C₃H₇

-86 n-C₃H₇

-87 n-C₆H₁₃

-88 n-C₃H₇

Example 2 Hydrogenation

General Working Procedure B2 (GWP B2)

Compound B1.2 (100 mmol) is dissolved in heptane, hydrogenation catalyst (10% platinum on activated carbon or 5% Pd/C) is added, and the compound is hydrogenated at a temperature between room temperature and 50° C. under a hydrogen partial pressure of 5 bar. The reaction solution is concentrated and filtered, and the crude product B2.1 is isomerised if necessary and chromatographed and subsequently distilled under reduced pressure and/or crystallized. The cis/trans isomerization is carried out either by stirring for two hours with 15 mol % of potassium tert-butoxide in N-methylpyrrolidone or using a Lewis acid, such as MgBr₂, in toluene at between −10° C. and room temperature or using a Brönsted acid, such as trifluoromethanesulfonic acid, at room temperature for 24 hours.

Some of the compounds prepared in accordance with GWP B2 are shown in Table B2. TABLE B2 Compound B 2.1 No. R^(B2) R^(B2) -1

-2

-3

-4 n-C₃H₇

-5 n-C₃H₇

-6

-7

-8 CH₃

-9 CH₃

-10 CH₃

-11

-12

-13 C₂H₅

-14 n-C₃H₇

-15 n-C₃H₇

-16 C₂H₅

-17 C₂H₅

-18 n-C₃H₇

-19 n-C₃H₇

-20 n-C₃H₇

-21 n-C₃H₇

-22 C₂H₅

-23 n-C₃H₇

-24 n-C₅H₁₁

-25 n-C₃H₇

-26 n-C₃H₇

-27 n-C₃H₇

-28 n-C₄H₉

-29 n-C₄H₉

-30 n-C₃H₇

-31 n-C₃H₇

-32 C₂H₅

-33 n-C₃H₇

-34 n-C₃H₇

-35 n-C₃H₇

-36 n-C₃H₇

-37 C₂H₅

-38 C₂H₅

-39 C₂H₅

-40 n-C₃H₇

-41 C₂H₅

-42 C₂H₅

-43 n-C₃H₇

-44 n-C₃H₇

-45 n-C₃H₇

-46 n-C₃H₇

-47 n-C₃H₇

-48 n-C₃H₇

-49 C₂H₅

-50 C₂H₅

-51 C₂H₅

-52 n-C₃H₇

-53 n-C₃H₇

-54 n-C₃H₇

-55 n-C₃H₇

-56 n-C₃H₇

-57

-58 n-C₃H₇

-59 n-C₃H₇

-60 n-C₃H₇

-61 n-C₃H₇

-62 CH₃

-63

-64 n-C₃H₇

-65 n-C₃H₇

-66

-67 n-C₃H₇

-68 n-C₃H₇

-69 n-C₅H₁₁

-70 C₂H₅

-71 C₂H₅

-72 n-C₄H₉

-73 n-C₃H₇

-74 n-C₃H₇

-75 C₂H₅

-76 C₂H₅

-77 n-C₅H₁₁

-78 n-C₄H₉

-79 n-C₇H₁₅

-80 n-C₄H₉

-81 n-C₅H₁₁

-82 n-C₃H₇

-83 CH₃

-84 n-C₄H₉

-85 n-C₃H₇

-86 n-C₃H₇

-87 n-C₆H₁₃

-88 n-C₃H₇

Example 3 Synthesis of Allyl Compounds of the Formula IV

Diethyl 4-trans-propyl-1-cyclohexylmalonate B3.1 (0.2 mol) in anhydrous dimethoxyethane is added dropwise to a suspension of sodium hydride (0.24 mol) in dimethoxyethane. The mixture is refluxed for 5 hours, and lithium aluminium hydride (0.5 mol) is then added at 0° C. The mixture is subsequently refluxed for a further 3 hours. After cooling to 0° C., ethyl formate, then water, aqueous sodium hydroxide solution and again water are added. The mixture is filtered, and the aqueous phase is extracted with tert-butyl methyl ether. The combined organic phases are dried and evaporated, and the residue is filtered through silica gel. Removal of the solvent gives the allyl alcohol B3.2. Yield: 76%.

4-Dimethylaminopyridine (0.4 mol) in tetrahydrofuran is added dropwise at 0° C. with stirring to a solution of p-toluenesulfonyl chloride (0.2 mol) and 2-(4-trans-propyl-1-cyclohexylallyl alcohol B3.2 (0.2 mol) in tetrahydrofuran. When the addition is complete, the mixture is allowed to warm to room temperature and is then refluxed for a further 12 hours. After cooling, the mixture is poured into a mixture of ice and concentrated hydrochloric acid. The organic phase is separated off, and the aqueous phase is extracted three times with tert-butyl methyl ether. The combined organic phases are dried and evaporated, and the residue is chromatographed on silica gel. The allyltosyl ester B3.3 is obtained as an oil. Yield: 87%. The corresponding allyl methanesulfonate can be prepared analogously using methanesulfonyl chloride and the corresponding allyl trifluoromethanesulfonate can be prepared analogously using trifluoromethanesulfonic anhydride.

The allyltosyl ester B3.3 (0.1 mol) is taken up in acetone and refluxed for 36 hours with lithium bromide (0.1 mol). After cooling, the precipitate is filtered off, the filtrate is evaporated, and the residue formed is filtered through silica gel. Evaporation gives 2-(4-trans-propyl-1-cyclohexylallyl bromide B3.4. Yield: 68%.

Compound B3.5 (0.553 mol) and potassium tert-butoxide (0.692 mol) are combined in toluene and stirred overnight at 80° C. After cooling, water is added, and the mixture is extracted with methyl tert-butyl ether. The organic phase is separated off, dried and evaporated. The residue is taken up in pentane and filtered through silica gel. Evaporation gives the allyl bromide B3.4. Yield: 73%.

2-(4-trans-Propyl-1-cyclohexyl)-1,3-dibromopropane B3.5 (0.5 mol) is stirred for 16 hours at 80° C. in toluene together with potassium tert-butoxide (1.25 mol). After cooling, water is added, tert-butyl methyl ether is added, and the mixture is extracted. The organic phase is dried and evaporated, and the residue is filtered through silica gel. 2-(4-trans-Propyl-1-cyclohexyl)allyl tert-butyl ether B3.6 is obtained as an oily product.

Yield: 68%.

Triphenylphosphine (0.4 mol) is suspended in acetonitrile and cooled to 10° C., and bromine (0.39 mol) is added at this temperature. The suspension is stirred for a further 1 hour, and propyldicyclohexylpropane-diol B3.7 (0.2 mol) is then added. The mixture is stirred overnight at room temperature and subsequently refluxed for 4 hours. After cooling to room temperature, water is added, and the mixture is extracted with petroleum ether. The organic phase is dried and evaporated, and the residue is filtered through silica gel. Evaporation gives propyldicyclohexylpropane dibromide B3.8. Yield: 94%.

The dibromide B3.8 (0.402 mol) and potassium tert-butoxide (0.503 mol) are mixed in toluene and stirred at 80° C. overnight. The mixture is cooled, water is added, and the mixture is extracted with methyl tert-butyl ether. The organic phase is dried and evaporated. The residue is filtered through silica gel. Evaporation gives the allyl bromide B3.9. Yield: 90%.

2-(4-trans-Propyl-1-cyclohexyl)allyl alcohol (0.2 mol) is stirred vigorously at room temperature for 24 hours with 105 g of active manganese dioxide in 350 ml of dichloromethane. The mixture is then filtered, the residue is washed with dichloromethane, and the organic phase is evaporated and filtered through silica gel with toluene/methyl tert-butyl ether. Yield of the acrolein B3.10: 64%.

The aldehyde B3.11 (0.321 mol) and N,N-dimethylmethyleneiminium chloride (Eschenmoser's salt; 0.321 mol) are suspended in dichloromethane. Triethylamine is then added dropwise at room temperature, and the mixture is stirred overnight. The mixture is extracted by shaking with water, the organic phase is separated off and evaporated in a rotary evaporator, the residue is taken up in heptane/methyl tert-butyl ether, and the solution is filtered through silica gel. Yield: 40%.

Example 4 Synthesis of Homoallyl Compounds of the Formula V

a) General Working Procedure B 4a (GWP B4a)

The aldehyde B 4.1, dissolved in 100 ml of THF, is added dropwise with gentle ice-cooling to 200 ml (2 mol) of allylmagnesium chloride in diethyl ether (Aldrich Co.), and the mixture is then stirred at room temperature for 4 hours. The reaction mixture is subsequently poured into 100 ml of 0.5N HCl and stirred for five minutes. The organic phase is separated off, and the aqueous phase is extracted twice with methyl tertbutyl ether. The combined organic extracts are rinsed with water; dried, filtered and evaporated. The crude product, obtained quantitatively, can be used directly in the subsequent reaction owing to its purity. b) General Working Procedure B 4b (GWP B 4b)

Allylmagnesium chloride (0.40 mol) in 400 ml of diethyl ether (Aldrich Co.) is added dropwise with external cooling to a solution of zinc bromide (0.4 mol) in 200 ml of THF at such a rate that the temperature is between 10 and 15° C. The resultant suspension is stirred at this temperature for a further 2 hours, before 0.4 mol of the aldehyde B 4.3, dissolved in 400 ml of diethyl ether, is added dropwise. The suspension is stirred at room temperature for a further 16 hours and then poured into 600 ml of 0.5N HCl. The organic phase is isolated, dried using sodium sulfate and evaporated. The crude product can be employed without further purification. Instead of zinc bromide, ClTi(i-propoxide)₃ can also be used for the transmetallation.

This reaction procedure with transmetallation is particularly suitable for the reaction of aldehydes which, besides the aldehydic carbonyl function, contain a functional group which is reactive towards Grignard reagents, such as a carboxylate or nitrile group.

Example 5 Synthesis of Compounds of the Formula II

a) General Working Procedure B 5a (GWP B5a) (For Compounds B 4.2 for which Z¹³, Z¹⁴ and Z¹⁵ are not CO₂)

0.4 mol of granulated sodium hydroxide is suspended in 200 ml, of THF at room temperature, and 2 ml of water, 0.4 mol of homoallyl alcohol B 4.2 and 0.02 mol of N-cetyl-N,N,N-trimethylammonium bromide are added at 25° C. with stirring. 0.4 mol of the allyl bromide is then added with stirring. The mixture is stirred at from 40 to 50° C. for 20 hours. A further 0.05 to 0.1 mol of allyl bromide is subsequently added to homoallyl alcohol B 4.2 which has not reacted according to TLC in order to complete the reaction after continued stirring (12 hours). After cooling, the mixture is poured into 500 ml of ice-water and extracted twice with methyl tert-butyl ether. The combined organic extracts are dried, evaporated and filtered through silica gel with heptane/toluene. The compounds B 5.1 are usually obtained as an oil. Yield: 70 to 95%.

b) General Working Procedure B 5b (GWP B5b)

0.46 mol of NaH (60% suspension in paraffin oil) is initially introduced in 200 ml of THF. The homoallyl alcohol B 4.2 (0.4 mol) in 200 ml of THF is added dropwise at a temperature between −10 and +20° C. Stirring is continued at between 20 and 30° C. until the evolution of hydrogen is complete. 0.4 mol of the allyl bromide in 200 ml of THF is then added dropwise at room temperature, and, depending on the result of the TLC check, the mixture is stirred at room temperature for from 12 to 48 hours. The reaction mixture is poured into ice-water, extracted with methyl tertbutyl ether, dried, evaporated and filtered through silica gel with heptane/toluene. c) General Working Procedure B 5c (GWP B5c)

Acrylic acid esters B 5.2 are prepared by process GWP B 5a or GWP B 5b, with the allyl bromide being replaced by the corresponding acid chloride.

Example 6 Physical Parameters of Compounds According to the Invention

Table B3 shows selected physical parameters of some compounds according to the invention which have been prepared by the procedures of the above examples. (The entries in the “Compound” column refer to the names given in Examples 1 to 5). TABLE B3 γ₁ m.p. cl.p. Compound Δn Δε [mPa · s] [° C.] [° C.] Phase transitions B1.2-1* 0.0640 12.8 205 48  21*** C 48 I B1.2-2* 0.0740 14.5 286 35  36*** C 35 N (10.3) I B1.2-3* 0.1060 12.1 562 98 217 C 98 N 217 I B1.2-4* 0.0560 13.3 203 74  3*** C 74 I B1.2-7* 0.0740 14.5 286 35  36*** C 35 N (10.3) I B1.2-8* −0.0142 7.5 62 C 62 I B1.2-9* 0.0520 14.8 99 89  25*** C 89 I B1.2-11* 0.0760 8.2 137 84  63*** C 84 SmB? 90 I B1.2-12* 0.0739 8.4 79  37*** C 79 SmB (74) I B2.1-1* 0.0710 12.2 182 57  62*** C 57 N (50.9) I B2.1-2* 0.0770 13.5 325 69  68*** C 69 N 70 I B2.1-3* 0.1020 11.8 582 113 256 C 113 N 256 I B2.1-4* 0.0599 14.1 136 71  32*** C 71 I B2.1-9* 0.0490 34.9 142 54  16*** C 54 I B2.1-11* 0.0810 8.5 149 37 106 C 37 SmB 93 N 106 I B2.1-13* 0.0475 14.0 140 72  14*** C 72 I B2.1-14* 0.1256 18.0 239 58  61 C 58 SmA (37) N 61 I B2.1-15* 0.0570 13.4 34  58 C 34 N 58 I B2.1-16* 0.1493 27.3 287 77  91 C 77 N 91 I B2.1-17* 0.0540 14.1 124 45  35*** C 45 N (35) I B2.1-18* 0.1390 9.4 84 232 C 84 N 232 I B2.1-19* 0.1370 10.7 47 238 C 47 SmB 91 N 238 I B2.1-20* 0.1291 15.7 725 60 207 C 60 SmB 81 N 207 I B2.1-21* 0.1071 17.3 176 64  13*** C 64 I B2.1-22* 0.1310 29.9 89  69*** C 89 N (77) I B2.1-23* 0.1254 12.7 225 43  44 C 43 N 44 I B2.1-24* 0.0568 11.8 216 39  75 C 39 N 75 I B2.1-25* 0.1364 29.7 70 102 C 70 N 102 I B2.1-26* 0.0580 35.6 75 27 −83*** C 27 I B2.1-27* 0.1231 34.9 457 81  83 C 81 N 83 I B2.1-28* 0.0623 11.5 106 SmB 81 N 106 I B2.1-29* 0.0689 9.1 −54 117*** C? −54 SmB 129 I B2.1-30* 0.1220 19.1 625 61 192 C 61 N 192 I B2.1-31* 0.1328 13.4 806 44 213 C 44 Sm? 45 B 213 I B2.1-32* 0.1422 10.1 116 54 106*** C 54 Sm? SmB 154 SmA 168 I B2.1-33* 0.1243 14.8 178 42  44*** C 41 I B2.1-34* 0.1256 18.0 239 58  61 C 58 SmA (37) N 61 I B2.1-35* 0.0599 14.1 136 71  32*** C 71 I B2.1-36* 0.0570 13.4 160 35  66 C 35 N 66 I B2.1-37* 0.1070 29.7 213 89  48*** C 89 I B2.1-38* 0.1493 27.3 287 78  92 C 78 N 92 I B2.1-39* 0.1159 14.5 130 52  17*** C 52 I B2.1-40* 0.1243 14.8 178 41  44*** C 41 I B2.1-41* 0.0475 14.0 140 72  14*** C 72 I B2.1-42* 0.1159 14.5 130 52  17*** C 52 I B2.1-43* 0.1430 9.6 189 50  99 C 50 SmA-1 (32) SmA-2 64 N 99 I B2.1-44* 0.1380 12.7 236 45  90*** C 45 SmA-1 68 SmA-2 118 I B2.1-45* 0.0780 9.1 178 −41 129 C −41 SmB 123 N 129 I B2.1-46* 0.0701 11.7 199 106 SmB 74 N 106 B2.1-47* 0.0688 9.7 187 41  96 C 41 SmB 51 N 96 I B2.1-48* 0.1384 19.7 74 198 C 74 N 198 I B2.1-49* 0.1157 12.3 28  25*** C 28 N (11) I B2.1-50* 0.1100 15.2 177 37  39 C 37 SmA (35) N 39 I B2.1-52* 0.1450 23.2 300 75 118 C 75 N 118 I B2.1-53** 0.1190 40.8 529 91  47*** C 91 I B2.1-54* 0.0800 28.2 128 32 −50*** C 32 I B2.1-57* 0.0550 23.7 241 87  20*** C 87 I B2.1-58* 0.1158 35.6 541 74 101 C 74 N 101 I B2.1-59* 0.1330 25.3 466 80 120 C 80 N 120 I B2.1-60* 0.1230 61.4 625 79  91 C 79 N 91 I B2.1-61* 0.1706 35.4 115 198 C 115 N 198 I B2.1-62* 0.0950 18.9 160 58 −30*** C 58 I B2.1-63* 0.0871 21.7 106 207 C 106 N 207 I B2.1-64** 0.1649 37.9 98 193 C 98 N 193 I B2.1-65* 0.0049 7.7 76 7 −78*** C 7 SmB 15 I B2.1-66* 0.0880 21.3 91 203 C 91 SmH (63) N 203 I B2.1-67** 0.1510 42.1 144 181 C 144 N 181 I B2.1-68* 0.1180 29.8 541 48 105 C 48 SmA (46) N 105 I B2.1-69* 0.1279 57.4 50  95 C 50 N 95 I B2.1-70* 0.1149 35.0 356 91  38*** C 91 N (59) I B2.1-71* 0.1202 64.0 536 77  38*** C 77 N (66) I B2.1-72* 0.1270 58.0 534 76  90 C 76 N 90 I B2.1-73** 0.1634 37.7 121 205 C 121 N 205 I B2.1-74** 0.1411 43.8 128 201 C 128 N 201 I B2.1-75** 0.1431 29.8 113 149 C 113 N 149 I B2.1-76* 0.1459 67.8 98 128 C 98 N 128 I B2.1-77* 0.1490 61.8 65 142 C 65 SmC (44) N 142 I B2.1-78* 0.1477 64.2 79 139 C 79 N 139 I B2.1-79* 0.1459 58.5 64 131 C 64 N 131 I B2.1-80* 0.1171 32.4 381 90  54*** C 90 N (81) I B2.1-81* 0.1205 31.9 589 82  89 C 82 N 89 I B2.1-82* 0.1130 30.3 662 83  86 C 83 N 86 I B2.1-83* 0.0459 14.5 126 72 −19*** C 72 I B2.1-84* 0.0960 16.4 185 55  14*** C 55 I B2.1-85* 0.2052 31.4 107 186 C 107 N 186 I B2.1-86* 0.1372 31.5 607 80 107 C 80 N 107 I B2.1-87* 0.1116 30.6 473 89  59*** C 89 N (83) I B2.1-88* 0.2125 59.4 121 269 C 121 N 269 *The parameters Δn, Δε and γ₁ are determined by measurement of a mixture of 10% by weight of the compound in the host ZLI-4792 (Merck KGaA, Darmstadt) followed by extrapolation. **The parameters Δn, Δε and γ₁ are determined with 5% by weight of the compound in ZLI-4792. ***The clearing point is determined by measurement of a mixture of 10 or 5% by weight of the compound in the host ZLI-4792 followed by extrapolation.

The entire disclosure[s] of all applications, patents and publications, cited herein and of corresponding German application No. 10324312.7, filed May 27, 2003 is incorporated by reference herein.

The preceding examples can be repeated with similar success by substituting the generically or specifically described reactants and/or operating conditions of this invention for those used in the preceding examples.

From the foregoing description, one skilled in the art can easily ascertain the essential characteristics of this invention and, without departing from the spirit and scope thereof, can make various changes and modifications of the invention to adapt it to various usages and conditions. 

1. A compound of formula I

wherein a, b, c, d and e are each, independently of one another, 0 or 1; W is —CH₂— or —C(═O)—; R¹¹ is H, an alkyl radical having from 1 to 15 carbon atoms optionally mono- or polysubstituted, identically or differently, by halogen or —CN, wherein optionally, one or more CH₂ groups in this radical may be replaced by —C≡C—, —CH═CH—, —O, —S—, —C(O)—O— and/or —O—C(O)— in such a way that hetero atoms (O and S) are not linked directly to one another; R¹² is H, halogen, —CN, —NCS, aralkyl, O-aralkyl or an alkyl radical having from 1 to 15 carbon atoms optionally mono- or polysubstituted, identically or differently, by halogen or —CN, wherein optionally, one or more CH₂ groups in this radical may be replaced by —C≡C—, —CH═CH—, —O—, —S—, —C(O)—Oand/or —O—C(O)— in such a way that hetero atoms (O and S) are not linked directly to one another; Z¹¹ is a single bond, —CH₂—, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂—, —CF₂CF₂—, —CH═CH— or —C≡C—; Z¹² is a single bond, —CH₂—, —CH₂CH₂—, —.CF₂CH₂—, —CH₂CF₂— or —CF₂CF₂—; Z¹³, Z¹⁴ and Z¹⁵ are each, independently of one another, a single bond, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂—, —CF₂CF₂—, —CH═CH—, —C≡C—, —CH₂O—, —CF₂O—, —C(O)— or —C(O)—O—; A¹¹ and A¹², independently of one another, are

A¹³ and A¹⁴, independently of one another, are

A¹⁵ is

or A¹⁵-R¹² together are

or Z¹³-[-A¹³-Z¹⁴-]_(c)-[-A¹⁴-Z¹⁵-]_(d)-[-A¹⁵-]_(e)-R¹² is

wherein L¹⁷, L¹⁸ and L¹⁹, independently of one another, are H or F; q is 0, 1, 2, 3 or 4; p is 0, 1, 2 or 3; R¹³ and R¹⁴, independently of one another, are an alkanyl radical having from 1 to 7 carbon atoms or together are an alkylene bridge having from 2 to 7 carbon atoms; with the proviso that, in the case of direct linking of Z¹³ and R¹² to give -Z¹³-R¹², R¹² is H, aralkyl, alkanyl or alkenyl if Z¹³ is —C(═O)—O— or —C(═O)—, and Z¹³ is not —CH₂O— or —CF₂O—; that, in the case of direct linking of Z¹⁴ and R¹² to give -Z⁴-R¹², R¹² is H, aralkyl, alkanyl or alkenyl if Z¹⁴ is —C(═O)—O— or —C(═O)—, and Z¹⁴ is not —CH₂O— or —CF₂O—; that, in the case of direct linking of Z¹⁵ and R¹² to give -Z¹⁵-R¹², R¹² is H, aralkyl, alkanyl or alkenyl if Z¹⁵ is —C(═O)—O— or —C(═O)—, and Z¹⁵ is not —CH₂O— or —CF₂O—; that R¹¹ is not H if simultaneously a and b are both zero and Z¹² is a single bond; that R¹¹ is not CH₃ if simultaneously a and b are both zero, Z¹² and Z¹³ are each a single bond, W is —CH₂— and -[-A¹³-Z¹⁴-]_(c)-[-A¹⁴-Z¹⁵-]_(d)-[-A¹⁵-]_(e)-R¹² is unsubstituted phenyl.
 2. A compound according to claim 1, wherein a+b+c+d+e≦3.
 3. A compound according to claim 1, wherein W is —C(═O)—.
 4. A compound according to claim 1, wherein W is —CH₂—.
 5. A compound according to claim 1, wherein Z¹² is a single bond.
 6. A compound according to claim 1, wherein b is 1; Z¹¹ is a single bond; and A¹² is


7. A compound according to claim 1, wherein a is 1; and A¹¹ is


8. A compound according to claim 1, wherein Z¹³ is a single bond, —C(O)—O— or —CF₂O—.
 9. A compound according to claim 1, wherein e is 1; A¹⁵ is

and L¹¹ and L¹², independently of one another, are H or F.
 10. A compound according to claim 1, wherein e is 1; A¹⁵-R¹² is


11. A compound according to claim 1, wherein c is 1; Z¹⁴ is a single bond, —C(O)—O— or —CF₂O—; A¹³ is

and L¹³ and L¹⁴, independently of one another, are H or F.
 12. A compound according to claim 1, wherein d is 1; Z¹⁵ is —CF₂O—; A¹⁴ is

and L¹⁵ and L¹⁶, independently of one another, are H or F.
 13. A process for the preparation of a compound according to claim 1, comprising a metathesis ring-closing of a compound of formula II

to give a compound of the formula I

in the presence of a metathesis catalyst.
 14. A process according to claim 13, wherein the metathesis catalyst is a ruthenium-alkylidene complex.
 15. A process according to claim 13, further comprising after the metathesis reaction step, reducing the compound of the formula I wherein W is —C(═O)— and Z¹³, Z¹⁴ and Z¹⁵ are not —C(O)—, into a compound of the formula I, wherein W is —CH₂—; R¹¹ is H, an alkyl radical having from 1 to 15 carbon atoms' optionally mono- or polysubstituted, identically or differently, by halogen or —CN, optionally one or more CH₂ groups in this radical may be replaced by —C≡C—, —CH═CH—, —O— and/or —S— in such a way that hetero atoms (O and S) are not linked directly to one another; R¹² is H, halogen, —CN, —NCS, aralkyl, O-aralkyl or an alkyl radical having from 1 to 15 carbon atoms, optionally mono- or polysubstituted, identically or differently, by halogen or —CN, optionally one or more CH₂ groups in this radical may be replaced by —C≡C—, —CH═CH—, —O— and/or —S— in such a way that hetero atoms (O and S) are not linked directly to one another; Z¹³, Z¹⁴ and Z¹⁵ are each, independently of one another, a single bond, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂—, —CF₂CF₂—, —CH═CH—, —C_C—, —CH₂O— or —CF₂O—.
 16. A process according to claim 13 further comprising after the metathesis ring-closing and conducting any reduction reaction, catalytically hydrogenating to obtain a compound of the formula III:

wherein f, g, h, j and k are each, independently of one another, 0 or 1; R³¹ is H, an alkyl radical having from 1 to 15 carbon atoms optionally mono- or polysubstituted, identically or differently, by halogen or —CN, wherein, optionally one or more CH₂ groups in this radical may be replaced by —O—, —S—, —C(O)—O and/or —O—C(O)— in such a way that hetero atoms (O and S) are not linked directly to one another; R³² is H, halogen, —CN, —NCS, aralkyl or an alkyl radical having from 1 to 15 carbon atoms optionally mono-or polysubstituted, identically or differently, by halogen or —CN, wherein optionally one or more CH₂ groups in this radical may be replaced by —O—, —S—, —C(O)—O— and/or —O—C(O)— in such a way that hetero atoms (O and S) are not linked directly to one another; Z³¹ and Z³², independently of one another, are a single bond, —CH₂—, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂— or —CF₂CF₂—; Z³³, Z³⁴ and Z³⁵ are each, independently of one another, a single bond, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂—, —CF₂CF₂—, —CH₂O—, —CF₂O—, —C(O)— or —C(O)—O—; A³¹ and A³², independently of one another, are

A³³ and A³⁴, independently of one another, are

A³⁵ is

or A³⁵ R³² together are

or Z³³-[-A³³-Z³⁴-]_(h)-[-A³⁴-Z³⁵-]_(j)[A³⁵]_(k)R³² is

wherein L 37, L³⁸ and L³⁹, independently of one another, are H or F; r is 0, 1, 2, 3 or 4; s is 0, 1, 2 or 3; R³³ and R³⁴, independently of one another, are an alkanyl radical having from 1 to 7 carbon atoms or together are an alkylene bridge having from 2 to 7 carbon atoms; with the proviso that, in the case of direct linking of Z³³ and R³² to give -Z³³-R³², R³² is H, aralkyl or alkanyl if Z³³ is —C(═O)—, R³² is aralkyl or alkanyl if Z³³ is —C(═O)—O—, and Z³³ is not —CH₂O— or —CF₂O—; that, in the case of direct linking of Z³⁴ and R³² to give -Z³⁴-R³², R³² is. H, aralkyl or alkanyl if Z³⁴ is —C(═O)—, R³² is aralkyl or alkanyl if Z³⁴ is —C(═O)—O—, and Z³⁴ is not —CH₂O— or —CF₂O—; that, in the case of direct linking of Z³⁵ and R³² to give -Z³⁵-R³², R³² is H, aralkyl or alkanyl if Z³⁵ is —C(═O)—, R³² is aralkyl or alkanyl if Z³⁵ is —C(═O)—O—, and Z³⁵ is not —CH₂O— or —CF₂O—; that R³¹ is not H if simultaneously f and g are both zero and Z³² is a single bond.
 17. A process according to claim 13, further comprising before the metathesis ring-closing, reacting a compound of the formula IV with a homoallyl compound of the formula V

to form the compound of the formula II

wherein X¹¹ is a leaving group.
 18. A process according to claim 17, wherein W is —CH₂—; and X¹¹ is chlorine, bromine, iodine or a sulfonic acid radical.
 19. An allyl compound of the formula IV-Bb

wherein a is zero and b is 1 or a is 1 and b is zero or a and b are both 1; X^(11a) is chlorine, bromine, iodine, a sulfonic acid radical, —OH, alkoxy or O-aralkyl, or X^(11a) is ═O; R¹¹ is H, an alkyl radical having from 1 to 15 carbon atoms optionally mono- or polysubstituted, identically or differently, by halogen or —CN, wherein optionally one or more CH₂ groups in this radical may be replaced by —C≡C—, —CH═CH—, —O—, —S—, —C(O)—O— and/or —O—C(O)— in such a way that hetero atoms (O and S) are not linked directly to one another; Z¹¹ is a single bond, —CH₂—, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂—, —CF₂CF₂—, —CH═CH— or —C≡C—; Z¹² is a single bond, —CH₂—, —CH₂CH₂—, —CF₂CH₂—, —CH₂CF₂— or —CF₂CF₂—; A¹¹ and A¹², independently of one another, are


20. An electro-optical display device, comprising a liquid crystalline medium, in turn comprising a compound according to claim
 1. 21. An allyl compound according to claim 19, wherein A¹¹ and A¹² are 1,4-cyclohexylene.
 22. An electro-optical display device, comprising a liquid-crystalline medium, in turn comprising a compound made by the process of claim
 16. 